Pharmacist-led Chronic Disease Management Evidence-based Synthesis Program
54
APPENDIX A. SEARCH STRATEGIES MEDLINE (OVID)
1. Pharmacists/ or pharmacist:.ti,ab.2. (pharmaceutical care or pharmaceutical services or community pharmac: or clinical pharmac:).ti,ab.3. 1 or 24. Patient care/ or patient care management/5. Collaborative care.mp. or exp patient care planning/ or intervention:.mp.6. Case management/ or case management.mp. or care management.mp7. Disease management/ or disease management.mp. or (disease adj3 prevent:).mp.8. (chronic disease adj3 management).mp.9. (chronic disease adj3 prevent:).mp.10. Chronic care improvement.mp.11. 4 or 5 or 6 or 7 or 8 or 9 or 1012. 3 and 1113. Chronic disease/14. (chronic adj3 condition:).mp.15. Exp pulmonary disease, chronic obstructive/16. Congestive heart failure.mp. or heart failure/ or exp heart failure/17. Dyslipidemia.mp. or exp dyslipidemia/18. Diabetes.mp.19. Hypertension.mp. or exp hypertension/20. Cancer.mp. or exp neoplasms/21. Kidney disease.mp. or kidney diseases/ or exp kidney diseases/ or kidney failure.mp.22. Chronic pain.mp.23. Depression.mp. or exp depressive disorder/24. 12 or 14 or 15 or 16 or 18 or 19 or 20 or 21 or 22 or 2325. Outpatient/ or outpatient:.mp. or outpatient.ti,ab.26. Ambulatory.mp.27. Assisted living facilities/ or assisted living.mp.28. Primary care:.mp.29. Primary health care/30. Community pharmac:.mp.31. Outpatient clinics, hospital/ or clinic.mp.32. Office visits/ or community health services/ or clinics.mp.33. 25 or 26 or 27 or 28 or 29 or 30 or 31 or 3234. 12 and 24 and 3335. Limit 34 to (English language and yr=”1995-current”)36. Limit 35 to “all child (0 to 18 years)”37. Limit 36 to “all adult (19 plus years)”38. 36 not 3739. 35 not 3840. Limit 39 to (meta analysis or systematic reviews)41. Limit 39 to (controlled clinical trial or randomized controlled trial)42. Comparative study/43. 39 and 4244. Control group.mp.45. (control: or compar: or random:).ti,ab.46. 44 or 4547. 39 and 4648. 41 or 43 or 47
Pharmacist-led Chronic Disease Management Evidence-based Synthesis Program
55
CINAHL 1. Pharmacist* OR MH pharmacists 2. (pharmaceutical W1 (care or service?)) OR ((community or clinical) W1 pharmac*) OR collaborative W1
care OR intervention* OR ((care or case) W1 management) 3. Disease N1 management OR disease N3 prevent* OR ((chronic W1 disease) N3 (management or
prevent*)) OR chronic W1 care W1 improvement 4. (MH “Case Management”) OR (MH “Disease Management”) 5. 2 or 3 or 4 6. Chronic N3 condition* OR congestive W1 heart W1 failure OR dyslipidemia OR diabetes OR hypertension
OR cancer 7. Kidney N1 disease* OR kidney N1 fail* OR chronic N1 pain OR depression 8. (MH “Kidney Diseases+”) OR (MH “Chronic Pain”) OR (MH “Depression+”) 9. 6 or 7 or 8 10. Outpatient* OR ambulatory OR assisted W1 living OR primary W1 care OR community W1 pharmac* OR
clinic? 11. (MH “Outpatients”) OR (MH “Ambulatory Care”) OR (MH “Ambulatory Care Facilities+”) OR (MH
“Assisted Living”) OR (MH “Primary Health Care”) OR (MH “Community Health Centers”) 12. 10 or 11 13. 1 and 5 14. (MH “Office Visits”) 15. Office W1 visit* 16. 12 or 14 or 15 17. 9 and 13 and 16 18. 9 and 13 and 16 (limiters- randomized controlled trials, Search modes-find all my search terms 19. “meta analysis” OR “systematic review” OR “controlled clinical trial” OR :comparative study” OR
“control group” OR control* OR compar* OR random* (limiters-randomized controlled trials, search modes- find all my search terms)
20. (MH “Meta Analysis”) OR (MH “Systematic review”) OR (MH “Clinical Trials+”) OR (MH “Comparative Studies”) OR (MH “Control Group”)
21. 19 or 20 22. 17 and 21 23. 18 or 22 24. 18 or 22 (limiters- published date: 19950101-20150131; English Language; Exclude MEDLINE records;
Human; Age Groups: All Adult, search modes-Find all my search terms)
COCHRANE LIBRARY 1. Pharmacist* 2. Pharmaceutical next (care or service) 3. Collaborative next care 4. Intervention* 5. (care or case) next management 6. Disease near management 7. Disease near prevent* 8. (chronic next disease) near (management or prevent*) 9. Patient care:kw 10. MeSH descriptor: [Chronic Disease] explode all trees 11. MeSH descriptor: [Patient Care Planning] explode all trees 12. #2 or #3 or #4 or #5 or #6 or #7 or #8 or #9 or #10 or #11 13. #1 and #12 14. Chronic near condition? 15. Congestive next heart next failure 16. Dyslipidemia or diabetes or hypertension or cancer? 17. Kidney next disease? 18. Kidney next fail* 19. Chronic next pain 20. Depression
Pharmacist-led Chronic Disease Management Evidence-based Synthesis Program
56
21. MeSH descriptor: [heart Failure] explode all trees 22. MeSH descriptor: [Pulmonary Disease, Chronic Obstructive] explode all trees 23. MeSH descriptor: [Dyslipidemias] explode all trees 24. MeSH descriptor: [Diabetes Mellitus] explode all trees 25. MeSH descriptor: [Neoplasms] explode all trees 26. MeSH descriptor [kidney diseases] explode all trees 27. MeSH descriptor: [depressive disorder] explode all trees 28. #14 or #15 or #16 or #17 or #18 or #19 or #20 or #21 or #22 or #23 or #24 or #25 or #26 or #27 29. #13 and #28 30. Outpatient? Or ambulatory or clinic? 31. Assisted near living 32. Primary next care 33. Community next pharmac* 34. Primary health care:kw 35. Outpatient clinics, hospital:kw 36. Office visits:kw 37. Community health services:kw 38. #30 or #31 or #32 or #33 or #34 or #35 or #36 or #37 39. #29 and #38
Publication Year from 1995 to 2015
INTERNATIONAL PHARMACEUTICAL ABSTRACTS (IPA) 1. pharmacists/ or pharmacist:.ti,ab. 2. (pharmaceutical care or community pharmacy or clinical pharmac:).ti,ab. 3. 1 or 2 4. patient care/ or patient care management/ 5. case management/ or case management.mp. or care management.mp. 6. patient education as topic/ or counsel:.mp. 7. disease management/ or disease management.mp. or (disease adj3 prevent:).mp. 8. medication therapy management/ or (medication adj3 management).mp. 9. (prescription adj3 management).mp. 10. medication optimiz:.mp. or drug interactions/ or therapeutic plan.mp. 11. prescription optimiz:.mp. 12. dt.fs. or drug therapy/ or medication counseling.mp. 13. prescription counseling.mp. 14. drug monitoring/ or prescription monitor:.mp. or drug monitor:.mp. 15. medication surveillance.mp. or medication reconciliation/ or prescription reconciliation.mp. 16. ((medication adj3 review) or (prescription adj3 review) or (drug adj3 review)).mp. 17. 4 or 5 or 6 or 7 or 8 or 9 or 10 or 11 or 12 or 13 or 14 or 15 or 16 18. 3 and 17 19. limit 18 to (english language and yr="1995 -Current") 20. limit 19 to journal articles 21. Comparative Study/ 22. control group.mp. 23. (control: or compar: or random:).ti,ab. 24. study design.ti,ab. 25. 22 or 23 or 24 26. 20 and 25 27. outpatient/ or outpatient:.mp. 28. ambulatory.mp. 29. urgent care.mp. 30. emergency:.mp. 31. assisted living facilities/ or assisted living.mp. 32. primary care:.mp. 33. community:.mp. 34. 27 or 28 or 29 or 30 or 31 or 32 or 33 35. 26 and 34
Pharmacist-led Chronic Disease Management Evidence-based Synthesis Program
57
APPENDIX B. PEER REVIEW COMMENTS/AUTHOR RESPONSES Reviewer Comments Export
Pharmacist-led Chronic Disease Management: A Systematic Review of Effectiveness and Harms Compared to Usual Care
Question Text Comment Response Are the objectives, scope, and methods for this review clearly described?
Yes Thank you Yes Yes Yes Yes Yes
Is there any indication of bias in our synthesis of the evidence?
No Thank you No Yes - only in the Executive Summary Please see below for our response Yes - Description of bias noted in review comments Please see below for our response No Thank you No
Are there any published or unpublished studies that we may have overlooked?
Yes - Based on your search strategy, I would have thought that a VA study which compared pharmacist-managed ESA clinic (for CKD) would have been included in the section of CKD. References below. (disclosure- I am one of the authors. Having said that, I really don't care if this study is included, if there is good reason why it should not be included.) 1. Aspinall SL, Cunningham FE, Zhao X, Boresi JS, Tonnu-Mihara IQ, Smith KJ, Stone RA, Good CB. Impact of pharmacist-managed erythropoiesis-stimulating agents clinics for non-dialysis chronic kidney disease patients. Am J Kidney Dis 2012; 60 (3): 371-9. PMID 22633556 2. Aspinall SL, Smith KJ, Good CB, Zhao X, Stone RA, Tonnu-Mihara IQ, Cunningham R, for the ESA Clinic Study Group. Incremental cost-effectiveness of pharmacist-managed erythropoietin-stimulating agent clinics for non-dialysis-dependent chronic kidney disease. Appl Health Econ and Health Policy 2013; 11:653-660.
Thank you for identifying this study. We have added the 2 articles to our review.
No No Yes - Recommendations noted in review comments. Thank you. Please see below for our response. No No
Pharmacist-led Chronic Disease Management Evidence-based Synthesis Program
58
Additional suggestions or comments can be provided below. If applicable, please indicate the page and line numbers from the draft report.
Three Comments 1) The report mentions in several sections the concern that while attaining many targets better in pharmacy intervention arms, compared to control- those targets have not been shown to improve clinical outcomes, and may actually be associated with harm. I find this somewhat curious- indeed, this is true. But, it is true in hindsight- at the time most of these studies were done, it was generally accepted that these targets were clinically relevant (for instance, that HBA1C of less than 7 was an important target). So, to criticize those intermediate outcomes seems unfair. Indeed, the pharmacists in those studies accomplished what they were asked to accomplish. Today, we would design those studies differently, but we have evidence that came after the referenced studies were done. Furthermore, the fact that most of the studies only demonstrate intermediate outcomes really reflects the roll of the clinical pharmacist in the clinic. Most of the studies were relatively short term, reflecting the reason patients are sent for clinical pharmacist input- usually goal directed (improve blood pressure control, etc). 2. I did not have time to pull individual articles, but I did pull several. Randomly, I looked at the Gattis article. It is published in a reputable journal. In the text, the study is referenced as showing no significant difference in clinical outcomes (overall mortality) but the study reports sig decrease in mortality plus heart failure events. If this outcome was not valid, I feel it should have been clear in the report that while the study reported a clinically relevant improvement in outcome, these were not accepted because of……(In the tables, it shows up under hospitalizations…being significantly less). 3. The review was also intended to evaluate harms. However, "harms" is almost never mentioned throughout the report. Harms are not specifically mentioned in the Executive Summary, and in the individual sections, adverse events are identified as a gap area. However, this is not clearly articulated as seeking evidence for "harms". Suggest explicitly discussing "harms"- which I assume that there is little evidence to address in the review.
1) We have limited our review to the findings of the studies, and rephrased our Limitations and Conclusions 2. The combination outcome from the Gattis article was reported on the Evidence Table in the Appendix but was not carried forward accurately to the report. We have made that change. 3. Although systematic reviews do have different criteria for evidence of harm, there was insufficient evidence on harms as most studies didn’t report harms and those that did often didn’t report data for the control group.
The information presented in the report is well constructed and comprehensive in its review of the topic. The research question is concise and well formulated. The summary and analysis of reviewed/considered data upon which an attempted answer to the question is based is objectively and accurately presented. As a reader/reviewer, I was generally able to understand the
Thank you. We have added some examples of “clinical events” in the listing of
Pharmacist-led Chronic Disease Management Evidence-based Synthesis Program
59
distinctions between various measured/evaluated parameters. However, the listing of one or two relevant examples of the authors' "definition" of "clinical events" (within a disease being examined) in relationship to the broader "clinical outcomes" of interest across all disease types (which are explicitly stated) would likely be helpful to future readers and users of the report. That is, what specific thing might qualify as an example of a "clinical event" in the care and treatment of a patient with the specified disease under scrutiny. Most other definitions, measures, and examples are more clearly detailed.
outcomes of interest and as a footnote to the Strength of Evidence tables..
My impression from this systematic review is that pharmacists are not yet good at designing studies and choosing or measuring the outcomes the reviewers deem important. It may be that pharmacist- led team have not been numerous enough or in existence long enough to reach important mortality end points. A more complete description of the evolution of pharmacists from product preparation to patient providers may be helpful. The papers they reviewed were very heterogeneous and not powered to detect the outcomes this review considered most important (e.g. mortality, resource use, access, satisfaction). Nevertheless, they show that pharmacist provided care is for the most part not different from non-pharmacist with goal attainment (LDL, HgbA1c, BP) being better with pharmacist provided care. In the executive summary these facts were presented in a very negative light. For example, on actual page 35, study page 23 paragraph 1 under key findings: they drew conclusions about pharmacist-led care not improving outcomes for depression but specifically stated “studies were not always adequately designed or analyzed for these outcomes”. If that is the case, state lack of study design but do not move to a broader conclusion. My global impression is that this systemic review including categorization, inclusion/exclusion etc. is sound but the way the results are interpreted and the wording of their summary/discussion/conclusion can be improved. The way it is now stated, can be misinterpreted and shed a negative light on what pharmacists have done to date. Specifically, the part on goal attainment which actually showed that pharmacists provided care did better in this category. But, this is undermined by saying that these goals are less strict now anyway and there isn’t a strong evidence that attaining these goals are clinically meaningful. While this may be true, it did not represent the evidence/guidance at the time which is a more global issue. Edits: Actual page 54, study page 41, paragraph 4, line 3: “further study is needed” change to- further studies are needed Actual page 38, study page 26, paragraph 4, line 4: “Two studied
We agree that published studies were not designed to assess mortality and clinical events or authors did not report these findings We would note that most of the included studies looked at the addition of pharmacist-led care to usual care, not pharmacist-led care versus non-pharmacist care. We have rephrased the conclusions about the depression studies. We have modified the wording of the Limitations and Conclusions sections. Edits: Thank you. We have made changes to these sentences.
Pharmacist-led Chronic Disease Management Evidence-based Synthesis Program
60
reported no significant differences” change to- Two studies reported The authors have conducted an extensive evidence-based review of Pharmacist-led Chronic Disease Management, particularly as it relates to effectiveness of care. The technical accuracy of the effectiveness of care review meets the evidence-based standards described in the report’s methodology. It is noted that the findings of this effectiveness of care review are similar to the 2014 systematic review of outpatient medication therapy management (MTM) interventions conducted by Viswanathan, et. al. (2014 AHRQ review). These similarities would be expected as both analyses used similar evidence-based criteria arriving at a conclusion of difficulty interpreting findings due to heterogeneity of services and interventions. The purpose of this review is to provide the authors, and the Veterans Health Administration, with suggestions and recommendations for improving this ESP review as it pertains to the methodology employed, and implications and applicability of the evidence-based findings contained in this review -First, it would be helpful to the reader to frame the findings of this review in the context of evidence-based reviews of physicians, and other health professionals, chronic disease management services. In its present state, there is no frame of reference or context for understanding the findings of this report. Are these results similar or different than other evidence-based findings of chronic disease management provided by other health care professionals, as well as team-based care? -Second is a critique of the Review of Harms. It is greatly appreciated that the report’s Conclusions highlight the importance of achieving patient-specific treatment goals by noting that; ‘studies of pharmacist-led care generally achieved intermediate target thresholds designed to achieve a “goal attainment” that should be done cautiously to provide patient-centered high value health care.’ This is the essence of comprehensive team-based medication management in an era of accountable health care. However, it is repeatedly stated in the report that, “achieving target goals for HbA1c, blood pressure, and cholesterol reported in the included studies have not been convincingly demonstrated to improve health outcomes but can increase harms and costs.” If this statement is to be made, the evidence supporting this finding needs to be presented. The authors will need to summarize the results of other studies in which achieving intermediate target thresholds can cause harms (e.g. A1c < 7% in the elderly, LDL < 70 mg/dl in octogenarians, etc.). In fact, unless additional evidence-based studies describing harms from aggressively achieving intermediate target thresholds can be described, then it is strongly recommended that the report title be corrected to remove the
1) Our findings were based on the available evidence regarding pharmacist-led clinics. Other disease management clinics also frequently use measures such as “goal attainment.” We believe we have assessed the most clinically relevant endpoints and initially discussed these with our Technical Expert Panel. There are few studies comparing pharmacist-led chronic disease management to other health care professionals. Thus, we hesitate to draw any conclusions about whether pharmacists provide more or less value. 2) We have modified the Limitations and Conclusions. Regarding harms, please see response above.
Pharmacist-led Chronic Disease Management Evidence-based Synthesis Program
61
word HARMS, because a systematic evidence-based review of harms is not apparent in this analysis.
-Third, is an inherent bias in the report pertaining to use of an outcome measure without a published taxonomy or official nomenclature. It is understood that the term, “Drug-related Problems” is commonly used in the literature, however there is no published classification system for this term. On the other hand, a published taxonomy of Drug Therapy Problems is available in the National Library of Medicine. One suggestion for improving the report is to utilize the four main published categories of Drug Therapy Problems (e.g. indication, effectiveness, safety, and convenience/adherence) to frame the analysis of drug-related problems. And one other item, on page 14, line 28 there is a statement in regards to the CKD RCT that “drug-related problems were not reported for the control group.” Without clarification this may be an irresponsible statement. No human subjects protection program or Institutional Review Board would approve a study in which drug therapy problems were identified in a control group without taking appropriate actions to resolve drug therapy problems in the control group of patients. In Medicine, this would be analogous to identifying a medical condition in a control patient and not doing anything about it.
-Fourth, it is noted that the evaluation approach employed in this analysis is deeply vested in experimental design that dominates the toolkit of evidence-based medicine. This evaluation approach has been summarized by Pawson and Tilley as an, OXO design: observe a system (O), introduce a perturbation/intervention (X) to some participants but not others, and then observe again (O). [1] Pawson and Tilley assert that when studies use the OXO paradigm to evaluate social programs (including most system improvements in medicine), the result is almost always “a heroic failure, promising so much and yet ending up in ironic anticlimax. The underlying logic seems meticulous, clear-headed and militarily precise, and yet findings seem to emerge in a typically non-cumulative, low-impact, prone-to-equivocation sort of way.” The usual conclusion and assertion from traditional OXO evaluations of quality-improvement efforts in health care is either that nothing works or that the results are inconsistent and more research is needed. [1] Dr. Don Berwick, former CMS Administrator and champion of the Science of Quality Improvement, has stated that the OXO paradigm most commonly applied in the traditional toolkit of evidence-based medicine is, “a powerful, perhaps unequaled, research design to explore the efficacy of conceptually neat components of clinical practice—tests, drugs, and procedures. For other crucially important learning purposes, however, it serves less well.” [2] The introduction of interprofessional and interdisciplinary
3) Our list of medication outcomes of interest was approved by ourTechnical Expert Panel members. We have defined our meaning of “drug-related problems” and removed the term “drug therapy problems” from the review.
We have modified the text so the statement about drug-related problems in the control group has been deleted. It would have been more accurate to state that the drug related problems in the control group were not reported in the manuscript.
4) We evaluated studies that were specifically designed to assess theeffectiveness of pharmacist-led chronic disease management. We included many study types including those often used in quality improvement initiatives (as many of these were). We disagree that we held pharmacist-led CDM to “too demanding” quality. Our charge was to conduct a systematic review focusing on the highest quality evidence available, ie, controlled clinical trials. Implementation should require evidence of effectiveness that exceeds harms and costs (ie, high value). The studies we reviewed did not provide convincing evidence about the value of pharmacist-led care.
Pharmacist-led Chronic Disease Management Evidence-based Synthesis Program
62
chronic care management systems for establishing a rational medication use system in which pharmacists work with patients to achieve their goals of therapy with zero tolerance for preventable medication harms is a complex, multicomponent intervention—essentially a process of social change. Pawson and Tilley claim that the reason the OXO model fails in this context is because, “experimentalists have pursued too single-mindedly the question of whether a program works at the expense of knowing why it works.” [1]
The fifth and final area of improvement relates to the implications and applicability of findings within the Veterans Health Administration system. This is to say, that it would be very helpful to address the, “so what question” of the report’s findings. In many of the VISN regions of the VA system, there are exemplary pharmacist-led chronic care advances and innovations supported by evidence of improved quality of care. One of the most important topics that is not addressed in this report is reducing pharmacist-led care process variations across the VA VISN’s. The science of continuous quality improvement (e.g. statistical process controls, run charts, etc.) provides the tools, techniques and measures to achieve this urgent national need in the care of this country’s Veterans. Thank you for the opportunity to serve as an external review for this Evidence-based Report. References: 1.) Pawson R, Tilley N. Realistic Evaluation. London, England: Sage Publications Ltd; 1997. 2.) Berwick DM. The Science of Improvement. JAMA. 2008;299(10):1182-1184. doi:10.1001/jama.299.10.1182.
5) We agree that implications and applicability are important,however, our purpose is to provide a review of evidence for VA policy makers. It is also outside of the scope of this review to address the question of variation in practice across VA VISNs. We highlighted studies conducted in the VA system and are not aware of any other evidence of improved quality of care.
This is excellent work. My only comment is that I continue to urge the authors to phrase their findings carefully to avoid giving the impression that pharmacist-led care has been shown not to improve outcomes such as mortality. Rather, as the aphorism goes, absence of evidence should not be construed as evidence of absence. That is, the studies have not been done to evaluate those outcomes. This should be made clear.
Thank you. We agree and have reviewed our wording to be clear on the absence of evidence for key outcomes.
This is a very thorough and well done report. Several comments:
1. Pg. 5, lines 11-12 It is important to clarify these statements to statethat in certain patients the more intensive treatment targets may cause harm, but not all patients as the statement reads now. Also, not all patients require less intensive treatment targets. Those recommendations apply to certain high-risk patients (especially in diabetes) whereas this statement implies that all patients would require less intensive targets.
Thank you.
1. We have modified this section.
Pharmacist-led Chronic Disease Management Evidence-based Synthesis Program
63
2. Pg. 19, Table 3, line 12 The 1 does not have a key correspondingwith this and I believe it should be a 'b' instead.
3. Pg. 23, line 24-25 This statements says there were 3 RCT's butlists 4 references and again in lines 38 & 39 it talks about 2 studies but lists 3 references. Clarification here would be helpful.
4. Pg. 28, Figure 6 The placement of this figure is a bit confusing as itis in the middle of the diabetes study discussion but it combines the lipids, hypertension and polypharmacy studies with the diabetes. It may make more sense to put at the end after review of each of those sections.
5. Pg. 29, line 54 The dyslipidemia heading lists 2 RCTs, 2 CCTs, and2 Cohort studies while the text discusses 7 studies (line 54).
6. Pg. 33, line 14 "in the" is written twice.
7. Pg. 39, lines 28-31. See comment #1 above as the same applies inthis section and also on Pg. 42, lines 21 & 22.
2. We have made the correction
3. The 3 RCTs were reported in 4 papers. We have clarified this at thestart of the paragraph.
4. We have placed Figure 6 in the Diabetes section because that iswhere the first reference to the figure is located. We again refer to Figure 6 in the lipids, hypertension, and polypharmacy sections.
5. We have corrected/clarified the count of studies for theDyslipidemia section.
6. Thank you, we have made this edit.
7. We have modified the wording on treatment targets throughout thereport.
Pharmacist-led Chronic Disease Management Evidence-based Synthesis Program
64
APPENDIX C. EVIDENCE TABLES Table 1. Study and Intervention Characteristics – Cardiovascular Disease Studies
Author, year Study design Type of Clinic*
Target Population
Duration of study/
follow-up
Inclusion/ Exclusion Criteria
Goal of Intervention
Primary Outcome
Type of pharmacist Pharmacist Intervention Comparator
intervention Collaboration
Cardiovascular Disease or Risk Factors for Cardiovascular Disease Taveira 201411
RCT
Cardio-vascular Risk Reduction Clinic (CRRC) at VAMC
Adults with cardio-vascular disease risk factors
12 months
Inclusion: -actively enrolled in the CRRC clinic (documented CVD or DM) -achieved discharge criteria(HbA1c <7%), BP (DM <140/80 non-DM <140/90), and LDL goals (<2.59 mmol/L))
Exclusion: -conditions that may limit long-term adherence to study visits -life-expectancy < 1 year
Maintenance of cardiovascular risk factor control once it has been obtained
Time to failure for guideline goals of HbA1c (failure is >7%) and blood pressure (with DM failure is >140/80 without >140/90) over 12-month study period
Clinical pharmacists who were diabetes core content experts and certified as diabetes educators
1) N=72-Education -Behavioral and pharmacological interventions -Individualized cardiovascular risk report card -Medications initiated or titrated -Individualized homework and behavior change goals -Coaching of self-care skills Mode/Frequency: -Group medical visits (120 minute sessions every 3 months for 1 year; facilitated by pharmacist) plus standard primary care 2) N=73-Assessed adherence -Titrated medications -Referred to nutrition or physical therapy as needed -Obtained vitals and lab parameters Mode/Frequency: -Quarterly CRRC individual clinic visits plus standard primary care (30 minute visit with clinical pharmacist every 2-6 weeks until cardiovascular risk control attained)
N=55 Standard primary care (3-4 visits per year with primary care provider; referrals for nutrition and physical therapy available)
Not reported
Pharmacist-led Chronic Disease Management Evidence-based Synthesis Program
65
Author, year Study design Type of Clinic*
Target Population
Duration of study/
follow-up
Inclusion/ Exclusion Criteria
Goal of Intervention
Primary Outcome
Type of pharmacist Pharmacist Intervention Comparator
intervention Collaboration
Irons 201212
Cohort (retro)
University Cardiol-ogy Group
High cardiac risk patients
Patients followed until at goal for several months
Inclusion: -CAD (history of MI, CABG, angioplasty, coronary stent placement, stable angina, evidence of ≥50% stenosis of any major coronary artery, or significant CAD risk equivalent) -baseline SBP >135 mmHg -age 40-85 years -established care with physician from group -≥2 visits with clinical pharmacists (intervention) or cardiologist (control) during study period Exclusion: -history of systolic heart failure (EF < 40%) -significant renal disease -documented non-adherence with appointments (<70% compliance)
Optimize HTN medication management to improve blood pressure control
Difference within and between the 2 groups in percentage of patients who obtained BP < 130/80 mmHg during last documented clinic visit within time frame evaluated
Clinical pharmacists
N=59 Collaborative care model; scheduled patient clinic appointments with clinical pharmacists -Adjustment of drug regimens (add, delete, or change HTN medications) -Change dosages of existing HTN medications -Obtain appropriate laboratory measurements -Provide limited physical assessment -Educate referred patients -Follow-up based on adverse events and blood pressure control
No specific formulary or algorithms used
Mode/Frequency: -Minimum of 2 visits with the clinical pharmacist -Initial visit, subsequent follow-up visits were scheduled within 1-4 weeks -If patient was at goal without complications they were scheduled for follow-up in 3 months
N=58 unmatched, met same inclusion criteria; usual care in same cardiology clinic
Cardiologist referred patients to HTN service at his discretion
Written collaborative practice agreements in place
Consulted for changes of non-hypertensive medications
Pharmacist-led Chronic Disease Management Evidence-based Synthesis Program
66
Author, year Study design Type of Clinic*
Target Population
Duration of study/
follow-up
Inclusion/ Exclusion Criteria
Goal of Intervention
Primary Outcome
Type of pharmacist Pharmacist Intervention Comparator
intervention Collaboration
Coronary Artery Disease Spence 201413
Cohort (retro)
Outpatient pharmacy clinical service of integrated health care service
Non-adherent diabetes mellitus or CAD patients with HbA1c or LDL-C outside clinical goals
1 year follow-up
Inclusion: -age ≥18 - pharmacy benefit ≥1 year before and 1 year after index date -included in diabetes or CAD registries - non-adherent (MPR < 0.80) on ≥1 oral medication for diabetes or dyslipidemia -HbA1c ≥8% or LDL-C ≥100 mg/dL Exclusion: -active insulin prescription -resided in skilled nursing facility >10 days or received hospice care during study period -declined consult
Improve medication adherence
Primary outcome not stated
Pharmacists who received training on diabetes and dyslipidemia, consultation methodology including motivational interviewing, and workflow training
109 pharmacists participated in OPCS consultations
N=359 with diabetes; N=1,121 with dyslipidemia Outpatient Pharmacy Clinical Service (OPCS); consult (B-SMART methodology) with patients meeting OPCS criteria during prescription pick-up -Identify barriers to medication non-adherence and solutions to these barriers -Motivate patients -Recommend adherence tools -Triage patient if needed to improve medication adherence and outcomes
Mode/Frequency: -One-time -Face-to-face
N=428 with diabetes; N=1,049 with dyslipidemia matched Usual care; 4 usual care patients matched to each intervention patient by age, gender, and disease (diabetes or dyslipidemia)
Not reported
Olson 200914
RCT
Non-profit HMO in urban area
Patients with prior coronary artery disease (acute MI, percutane-ous coronary intervention, or coronary artery bypass graft surgery)
2 years
Inclusion: -required only yearly follow-up per CPCRS protocol -≥2 consecutive LDL-C and non-HDL-C values at goal (1 measure within 6 months of enrollment) -controlled blood pressure within 6 months Exclusion: -HbA1c ≥9% in past 6 months -dementia -death within 30 days of randomization -life expectancy <3 years
Maintain lipid control following discharge from cardiac disease management program
% of patients maintaining LDL-C goal at study end
Clinical pharmacy specialists
N=214 -Pharmacists telephoned patients to review results of annual fasting lipid profile, blood pressure measurements, and medications and adherence -Counsel on diet and exercise -Make medication adjustments to maintain treatment goals -Order follow-up lab tests -Patients scheduled for follow-ups and notified of results
Mode/Frequency: -Telephone -Letters informing patients of test results -Scheduled for follow-up fasting lipid profile
N=207 Usual care; fasting lipid profile ordered for 1 year in future; results to be returned to physician who addressed results and ordered follow-up tests as needed; laboratory reminders sent
Intervention patient contacts were documented in EMR for other healthcare providers to review
Pharmacist-led Chronic Disease Management Evidence-based Synthesis Program
67
Author, year Study design Type of Clinic*
Target Population
Duration of study/
follow-up
Inclusion/ Exclusion Criteria
Goal of Intervention
Primary Outcome
Type of pharmacist Pharmacist Intervention Comparator
intervention Collaboration
Congestive Heart Failure (CHF) Murray 200716
RCT
University-affiliated inner-city ambula-tory care
Low income patients with CHF
12 months (9 months active intervention, 3 months post-intervention assessment)
Inclusion: -age 50 and older -receive all care (including medications) through same health care system -diagnosis of CHF confirmed by primary care physician -regularly used at least 1 medication for HF -did not use or were not planning to use medication container adherence aid -access to working telephone -hearing in normal range -clinically stable Exclusion: -dementia
Improve adherence to CHF medications, reduce exacerbations requiring ED visits or hospitalizations, improve disease-specific QOL, increase patient satisfaction, reduce health care costs
Medication adherence and clinical exacerbations requiring ED visit or hospitalization
Trained by inter-disciplinary team (pharmacist, physician, geriatrician) with guidelines for treating CHF, key concepts in pharmaceu-tical care of older adults, communica-tion techniques, and pharma-cotherapy of drugs for CHF
N=122 -Protocol for intervention based on problem (eg, low medication adherence, knowledge) -Baseline medication history assessment of patient knowledge and skills -Patient-centered verbal instruction and written materials about medications (each medication category assigned an icon) -Monitoring of medication use, health care encounters, body weight, other relevant data -Communicated, as needed, with clinic nurses and primary care physicians
Mode/Frequency: -Baseline interview at enrollment, not with pharmacist -Verbal and written instructions when dispensing medications
N=192 (intentionally randomized more to usual care) Usual care; received prescription services from pharmacists who did not receive specialized training
Information about patients was communicated as needed to clinic nurses and PCPs
Pharmacist-led Chronic Disease Management Evidence-based Synthesis Program
68
Author, year Study design Type of Clinic*
Target Population
Duration of study/
follow-up
Inclusion/ Exclusion Criteria
Goal of Intervention
Primary Outcome
Type of pharmacist Pharmacist Intervention Comparator
intervention Collaboration
Gattis 1999(PHARM study)15
RCT
General cardiology faculty clinic
Heart failure (HF)
24 weeks/ median follow-up 6 months
Inclusion: -diagnosis of HF based on signs and symptoms of HF and Left Ventricle EF<45% Exclusion: -life expectancy <6 months -current participant in investigational drug trial -resident of skilled nursing facility -marked dementia or another psychological disorder preventing patient education and follow-up
Optimize HF therapy (including use and dose of ACE inhibitors or alternatives, avoiding digoxin toxicity, avoiding contraindicated drugs or drug interactions, recommending other medication changes)
Combined all-cause mortality and heart failure, clinical events
Clinical pharmacist
N=90 -Questionnaire to assess symptoms and response to therapy -Discussed patient’s case and verbally provided therapeutic recommendations regarding optimization of therapy to attending physician -Recommendations based off patient interview, history, and current drug regimen -Discussed changes in drug therapy with patient (purpose of each drug, importance of adherence) -Provided written information on directions for use and potential adverse events -Provided patients with telephone number to contact if questions or problems -Telephone follow-up at 2, 12, and 24 weeks with instruction to contact physician if continued or worsening symptoms (pharmacist also contacted physician to discuss these cases)
Mode/Frequency: -Telephone follow after initial clinic visit -Written information on medication -Provided telephone number to contact if questions or problems -Clinical pharmacist discussed changes made in drug therapy with the patient
N=91 Usual care (no pharmacist recommenda-tions or patient education; physician and/or physician assistant/nurse practitioner did patient assessment and education) -Pharmacist contacted patients at 12 and 24 weeks to identify clinical events
Attending physician, nurses, social workers, dietitians -Discussed patient’s case and verbally provided therapeutic recommendations regarding optimization of therapy to attending physician
*Record whether primary care or specialty, if academic affiliated, if rural or urbanCHF = congestive heart failure; CPCRS = Clinical Pharmacy Cardiac Risk Service; ED = emergency department; EMR = electronic medical record; HF = heart failure; LDL-C = low-density lipoprotein cholesterol; EF = ejection fraction; HDL-C = high-density lipoprotein cholesterol; QOL = quality of life; TSH = thyroid-stimulating hormone; CAD=coronary artery disease; HTN=hypertension; HbA1c=glycosylated hemoglobin; ACE=angiotensin converting enzyme; BP=blood pressure; ESRD=end stage renal disease; DRP=drug related problem
Pharmacist-led Chronic Disease Management Evidence-based Synthesis Program
69
Table 2. Drug-related Problems Outcomes – Cardiovascular Disease Studies
Study Intervention (n) Control (n)
Inappropriate dosage/prescription
or omission % (n/N)
Ineffectiveness% (n/N) Drug-drug or drug-disease interaction (describe) % (n/N)
Non-adherence to prescribed regimen % (n/N)
Clinical/adverse event % (n/N)
Pharmacy component Control Pharmacy
component Control Pharmacycomponent Control Pharmacy
component Control Pharmacy component Control
Cardiovascular Disease or Risk Factors for Cardiovascular Disease No studies reporting
Coronary Artery Disease Spence 201413 IG=1,121 CG=1,049
NR NR NR NR NR NR Adherence at 1 year MPR 0.70
% adherent 37 (419/1121)
MPR 0.74 (P=.003 vs
pharm) % adherent
38 (403/1049) (P=.62 vs pharm)
NR NR
Olson 200914 IG=214 CG=207
NR NR NR NR NR NR Persistence with lipid-lowering
therapy 86.5%
85.5% (P=.78)
Coronary Event 3.3%
5.8% (P=.21)
Congestive Heart Failure Gattis 199915 IG=90 CG=91
Fraction of target ACE
inhibitor dosea
1.0 (0.5, 1.0)
0.5 (0.19, 1)
(P<.001)
NR NR NR NR NR NR NR NR
Murray 200716 IG=122 CG=192
NR NR NR NR NR NR “Taking adherence”
during intervention
79% (71% at follow-up)
“Scheduling adherence”
during intervention
53% (49% at follow-up)
“Refill adherence” during study period 109%
68% (67% during follow-
up)
47% (49% during follow-
up)
105% P=.007
Adverse event or
medication error
38% (42/112)
47% (91/192) (P=.11)
a Median (25th, 75th percentiles)
Pharmacist-led Chronic Disease Management Evidence-based Synthesis Program
70
CG = control group; IG = intervention group; MPR = medication possession ratio; NR = not reported
Pharmacist-led Chronic Disease Management Evidence-based Synthesis Program
71
Table 3. Mortality, Quality of Life, Access, and Patient Satisfaction Outcomes – Cardiovascular Disease Studies
Study; Intervention (n) Control (n)
All-cause mortality % (n/N)
Health-related quality of life (describe)
Access to care (describe)
Patient satisfaction with care (describe)
Pharmacy component Control Pharmacy
component Control Pharmacy component Control Pharmacy
component Control
Cardiovascular Disease or Risk Factors for Cardiovascular Disease
No studies reporting
Coronary Artery Disease Olson 200914 IG=214 CG=207
8.4% 7.7% (P=.80)
NR NR NR NR NR NR
Congestive Heart Failure Gattis 199915 IG=90 CG=91
3% (3/90)a 5% (5/91)a
OR 0.59 (95% CI
0.12, 2.49) (P=.48)
NR NR NR NR NR NR
Murray 200716 IG=122 CG=192
NR NR Disease specific,
improvement from
baseline 6 months:
0.28 12 months:
0.39
6 months: 0.21
(P=.52) 12
months: 0.24
(P=.21)
NR NR Satisfaction with pharmacy
services, improvement from baseline to 12 months:
1.0
0.7 (P=.02)
a Primary outcome was all-cause mortality and nonfatal heart failure; OR 0.22 (95% CI 0.06, 0.63); P=.005 CG = control group; IG = intervention group
Pharmacist-led Chronic Disease Management Evidence-based Synthesis Program
72
Table 4. Healthcare Utilization and Cost Outcomes – Cardiovascular Disease Studies
Study; Intervention (n) Control (n)
Office visits Urgent care visits/
Emergency room (ER) visits
Hospitalizations Medications Costs or Other (describe)
Pharmacy component Control
Pharmacy component Control
Pharmacy component
Control Pharmacy
component Control Pharmacy
component Control Cardiovascular Disease or Risk Factors for Cardiovascular Disease Taveira 201411 IG=73 Individual IG=72 Group CG=55
Mean # of PCP visitsa (SD) Individual: 2.8 (1.1) Group:
3.0 (1.2)
2.8 (1.0) (P=.46 overall)
Mean # of visitsa
Individual: 0.4 (0.8) Group:
0.6 (1.0)
0.6 (1.1) (P=.35)
Mean # of visitsa
Individual: 0.3 (0.7) Group:
0.4 (0.8)
0.2 (0.5) (P=.18 overall)
Individual: no change in cholesterol
(0.9 to 1.1), BP (2.3 to 2.4), or
antihyper-glycemic meds
(1.9 to 1.9) from baseline
Group: increase in BP (2.1 to 2.3) and
antihyper-glycemic meds
(1.7 to 1.8) from baseline
(P<.05)
Decrease in cholesterol (1.3 to 1.2)
and antihyper-glycemic meds
(1.9 to 1.8) from baseline
(P<.05)
NR NR
Irons 201212 IG=59 CG=58
Clinic visits or BP assessment
(outside of scheduled
appointments) per year of follow-up
10.7 (9.52, 12.09)
3.45 (3.01, 4.12)
P<.0001
NR NR NR NR Number of anti-
hypertensive agents
(median) 3.0 (3.0, 4.0)
2.0 (2.0, 3.0) P=.0001
NR NR
Coronary Artery Disease Spence 201413 IG=1,121 CAD CG=1,049 CAD
NR NR 1-year follow-up
4.6% (51/1121)
4.5% (47/1049) (P=.94 vs pharm)
1-year follow-up
1.3% (15/1121)
2.1% (22/1049) (P=.17 vs pharm)
NR NR Cost savings (system)b
$11,640,296 Cost of
program: $1,713,468
Approximately $5.79 saved for every $1
spent on program
NR
Pharmacist-led Chronic Disease Management Evidence-based Synthesis Program
73
Study; Intervention (n) Control (n)
Office visits Urgent care visits/
Emergency room (ER) visits
Hospitalizations Medications Costs or Other (describe)
Pharmacy component Control
Pharmacy component Control
Pharmacy component
Control Pharmacy
component Control Pharmacy
component Control Olson 200914 IG=214 CG=207
NR NR NR NR 33.6% 27.1% (P=.14)
NR NR NR NR
Congestive Heart Failure Gattis 199915 IG=90 CG=91
NR NR NR NR Re-admission
rate 29%
Re-admission
rate 42%
P=.03
Receiving ACE inhibitor at follow-up
87% (78/90) Receiving ACE
alternative 75% (9/12)
79% (72/91) (P=.18)
26% (5/19) (P=.02)
NR NR
Murray 200716 IG=122 CG=192
NR NR All-cause 2.2 (3.3)
Heart failure 0.3 (1.0)
2.7 (4.9) IRR 0.82
(0.70, 0.95)
0.3 (1.3) IRR 1.09
(0.42, 2.87)
All cause 0.8 (1.7)
Heart failure 0.1
(0.5)
1.0 (1.8) IRR 0.81
(0.64, 1.04)
0.2 (0.6) IRR 0.77
(0.28, 2.10)
NR NR Total outpatient
costs (mean) $5483 (SD
$6434)
Total inpatient costs (mean) $5550 (SD
$13847)
$6373 (SD
$6501)
$7827 (SD
$20413)
a Results are for patients with diabetes only (n=178 of 200 patients enrolled) b From reduced ER visits and hospitalizations for DM and CAD patients CG = control group; IG = intervention group
Pharmacist-led Chronic Disease Management Evidence-based Synthesis Program
74
Table 5. Goal Attainment Outcomes – Cardiovascular Disease Studies
Study; Intervention (n) Control (n)
Patient Goal Attainment definition Percentage of patients attaining goal (n/N)
Pharmacy component Control Cardiovascular Disease or Risk Factors for Cardiovascular Disease Taveira 201411 IG=73 Individual IG=72 Group CG=55
Maintenance of HbA1c ≤ 7%, BP ≤140/80 mmHg, LDL cholesterol ≤ 2.59 mmol/l
HbA1c failure rates per quartera (95% CI) Individual: 0.24 (0.18, 0.33)
(/156 person-quarters) Adj HR (vs control) 0.34 (0.21, 0.53)
Group: 0.36 (0.28, 0.47) (/129 person-quarters)
P=.07 to individual Adj HR (vs control) 0.49 (0.32, 0.75)
BP failure rates per quartera Individual: 0.22 (0.16, 0.30)
(/166 person-quarters) Adj HR (vs control) 0.43 (0.27, 0.68)
Group: 0.31 (0.23, 0.41) (/140 person-quarters)
Adj HR (vs control) 0.62 (0.41, 0.95) LDL guideline adherenta
Individual: 75.0% Group: 88.5%
HbA1c: 0.82 (0.69, 0.96)
(/60 person-quarters) (P<.001 compared to intervention)
BP: 0.53 (0.40, 0.71)
(/87 person-quarters) (P<.002)
LDL adherent: 84.3% (P=.12)
Irons 201212 IG=59 CG=58
Blood pressure < 130/80 mmHg (Note: goal was not specified for the control group)
49% (29/59) 31% (18/58) (P=.0456)
Coronary Artery Disease Olson 200914 IG=214 CG=207
LDL < 100 mg/dL non-HDL <130 mg/dL diabetes, multi-vessel coronary disease, at least 1
recurrent coronary event, or current smoker had LDL goal < 70 mg/dL non-HDL goal <100 mg/dL
Blood pressure < 140/90 mmHg diabetes or chronic kidney disease had goal < 130/80 mmHg
LDL < 100 mg/dL: 91.0% LDL < 70 mg/dL: 68.6%
Non-HDL-C 88.7%
BP < 140/90 mmHg: 75.0% BP < 130/80 mmHg: 60.0%
LDL < 100 mg/dL: 93.1% (P=.46) LDL < 70 mg/dL: 56.8% (P=.23)
Non-HDL-C 88.2% (P=.89)
BP < 140/90 mmHg: 84.2% (P=.03) BP < 130/80 mmHg: 54.5% (P=.71)
Congestive Heart Failure
No studies reporting a Results are for patients with diabetes only (n=178 of 200 patients enrolled); results for patients without diabetes (n=22) were described narratively due to small number of patients per group CG = control group; IG = intervention group
Pharmacist-led Chronic Disease Management Evidence-based Synthesis Program
75
Table 6. Study and Intervention Characteristics – Chronic Kidney Disease Studies
Author, year Study design Type of Clinic
Target Population
Duration of study/
follow-up
Inclusion/ Exclusion Criteria
Goal of Intervention
Primary Outcome
Type of pharmacist Pharmacist Intervention Comparator
intervention Collaboration
Cooney 201520
RCT
CBOCs within Cleveland VA
Patients with CKD
Study period was 1 year; patients were called before appointment and after (with lab results, etc.)
Inclusion: -moderate to severe CKD (eGFR<45) -GFR<60 between 90 days and 2 years prior -≥1 primary care visit in year prior to study
Exclusion: -ESRD -ever referred for hospice care -<18 or >85 years old
Improve CKD care
Last clinical systolic BP for patients with poorly controlled HTN at baseline
Clinical pharmacists with ability to order and review labs and prescribe medications
N=1070 -Delivery system redesign: a. engaging pharmacists to interact withpatients and collaborate electronically with PCPs b. self-management support for patients(informational pamphlet) c. CKD registry to identify patients with CKDnot receiving guideline adherent care, for decision support during phone call, and to facilitate documentation of intervention -Phone contact prior to appointment to discuss CKD, HTN -Reviewed medications and lifestyle modifications, ordered recommended labs, arranged nephrology consults if severe CKD -Called patients to review abnormal results and initiate appropriate non-HTN medication changes -Recommended HTN management tactics to PCPs Mode/Frequency: -Phone-based, 2 calls
N=1129 Usual care from PCPs
Recommendations for HTN management given to PCPs in progress notes
Pharmacist-led Chronic Disease Management Evidence-based Synthesis Program
76
Author, year Study design Type of Clinic
Target Population
Duration of study/
follow-up
Inclusion/ Exclusion Criteria
Goal of Intervention
Primary Outcome
Type of pharmacist Pharmacist Intervention Comparator
intervention Collaboration
Aspinall 2012/2013 21,22
Historical cohort
16 VA Medical Centers
Receiving ESAs for NDD-CKD
6 month follow-up
Inclusion: -50 randomly selected outpatients from each site -NDD-CKD defined as eGFR<60 mL/min/1.73m2 -receiving ESA on long-term basis
Compare quality of ESA prescribing and monitoring with and without pharmacist- managed clinics
Quality of ESA prescribing, (ie, proportion of hemoglobin values within 10-12g/dL)
Pharmacists with scope of practice that allowed them to dose and monitor ESA therapy
N=314 (10 clinics) NOTE: an additional 91 patients categorized as receiving usual care at ESA clinic sites -Independently dose and monitor ESAs (guidelines in place)
Mode/Frequency: Not reported
N=167 (6 clinics) -Usual care (physician-based)
None reported
Pai 200918
Pai 200917
RCT (pilot)
Non-profit university-affiliated dialysis clinic
ESRD patients
2 years
Inclusion: -English speaking ->18 years old -stable hemodialysis regimen for ≥3 months
Effect of pharmaceutical care on DRPs, drug use, drug costs, hospitaliza-tions
Primary: change in quality of life (Renal Quality of Life Profile – RQLP)
Nephrology-trained clinical pharmacist or pharmacists completing post-doctoral training in nephrology pharmaco-therapy
N=57 (30/57 [53%] did not complete study) -One-on-one in-depth drug therapy review conducted by clinical pharmacist -At meetings approximately every 8 weeks: -patient interview -generate drug therapy profile -identify and address DRPs -provide health care provider and patient education -review labs Mode/Frequency: -In clinic, one-on-one -Every 8 weeks during the 2 year study period
N=47 (21/47 [45%] did not complete study) Usual care (brief drug therapy reviews by dialysis nursing staff as mandated by clinic policy)
Physician, fellow, nurse, social worker, dietitian involved in monthly formal patient reviews -pharmacist gave provider education
Pharmacist-led Chronic Disease Management Evidence-based Synthesis Program
77
Author, year Study design Type of Clinic
Target Population
Duration of study/
follow-up
Inclusion/ Exclusion Criteria
Goal of Intervention
Primary Outcome
Type of pharmacist Pharmacist Intervention Comparator
intervention Collaboration
Bucaloiu 200719
Retro cohort
Nephrol-ogy clinic
Anemia of CKD
Minimum of 6 months; maximum of 1 year
Inclusion: -adults -anemia of CKD -treated with outpatient EPO -followed for ≥6 months
Exclusion: -managed by hematology-oncology or another nephrology group -on dialysis
Clinical and economic benefits
Primary outcome not specified
NR N=62 Protocol-driven pharmacist-managed program to manage anemia of CKD
Received epoetin alfa and sucrose intravenously per protocol
Mode/Frequency: -Patients followed between 6 months and 1 year -Hemoglobin/iron saturation measured at least monthly
N=74 matched Managed by PCPs (no protocol or pharmacist oversight)
Received epoetin alfa
NR
CG = control group; CKD = chronic kidney disease; DRP = drug-related problem; EPO = epoetin alfa; ESA = erythropoiesis-stimulating agents; ESRD=end stage renal disease; HTN = hypertension; IG = intervention group; NDD = non-dialysis-dependent; NR = not reported; PCP = primary care physician
Pharmacist-led Chronic Disease Management Evidence-based Synthesis Program
78
Table 7. Drug-related Problems Outcomes – Chronic Kidney Disease Studies
Study Intervention (n) Control (n)
Inappropriate dosage/prescription
or omission % (n/N)
Ineffectiveness% (n/N) Drug-drug or drug-disease interaction (describe) % (n/N)
Non-adherence to prescribed regimen
% (n/N) Clinical/adverse events
% (n/N)
Pharmacy component Control
Pharmacy component Control
Pharmacy component Control
Pharmacy component Control
Pharmacy component Control
Cooney 201520 IG=1,070 CG=1,129
NR NR NR NR NR NR Medication Adherence
6.8 (1.2)
6.7 (1.2) P=.70
NR NR
Aspinall 2012/201321,22 IG=314 CG=67 (Additional 91 patients receiving usual care at ESA clinic)
NR NR NR NR NR NR NR NR Thrombo-embolisma
n=6 (0.02/180 pt-days)
Heart Failureb
n=18 (0.06/180 pt-days) Uncon-trolled HTNc
n=185 (0.66/180 pt-days)
Thrombo-embolism
n=7 (0.05/180 pt-days)
Heart Failure
n=9 (0.06/180 pt-days)
HTN n=73 (0.48/180 pt-days)
All “clinically similar”
Pai 200918 IG=57 CG=47
Sub-therapeutic dosage:
14% of 530 DRPs identified
Untreated indication:
25%
NR NR NR NR NR NR NR Overdose: 5% of 530
DRPs identified
NR
Bucaloiu 200719 IG=62 CG=74
NR NR NR NR NR NR NR NR NR NR
CG = control group; DRP = drug-related problem; HTN = hypertension; IG = intervention group; pt-days = patient days a Thromboembolic event (myocardial infarction, stroke, deep vein thrombosis, pulmonary embolism) resulting in an emergency department visit or hospitalization b Resulting in an emergency department visit or hospitalization c Systolic blood pressure > 160 mmHg or diastolic blood pressure > 100 mmHg
Pharmacist-led Chronic Disease Management Evidence-based Synthesis Program
79
Table 8. Mortality, Quality of Life, Access, and Patient Satisfaction Outcomes – Chronic Kidney Disease Studies
Study; Intervention (n) Control (n)
All-cause mortality % (n/N)
Health-related quality of life (describe)
Access to care (describe)
Patient satisfaction with care (describe)
Other Outcomes
Pharmacy component Control Pharmacy
component Control Pharmacy component Control
Pharmacy component Control
Cooney 201520 IG=1,070 CG=1,129
50/1070 4.7%
74/1129 6.6% P=.06
No sig diff between intervention and control for
SF12MCS, SF12PCS, KDQOL Burden, KDQOL
Effects
NR NR 92% of participants surveyed
felt pharmacists provided
useful information and would
recommend program to
others
NR NR
Pai 200917,18 IG=57 CG=47
15/57 26% 12/47 26% Total RQLP Baseline: 71.9 (40)
1 year 71.4 (33.6)
2 years 56.5 (32.6)
Baseline: 74.5
(33.5) 1 year
ES 0.08 87.5
(30.4)a
ES 0.53 2 years
68.8 (35.8)
ES 0.34
NR NR NR NR NR
a P<.05 vs pharmacist intervention CG = control group; ES = effect size; IG = intervention group; KDQOL = Kidney Disease Quality of Life; NR = not reported; RQLP = renal quality of life profile (higher score = worsening quality of life); SF12 = Short Form; MCS = mental component score; PCS = physical component score
Pharmacist-led Chronic Disease Management Evidence-based Synthesis Program
80
Table 9. Healthcare Utilization and Cost Outcomes – Chronic Kidney Disease Studies
Study; Intervention (n) Control (n)
Office visits Urgent care visits/
Emergency room (ER) visits
Hospitalizations Medications Costs or Other (describe)
Pharmacy component
Control
Pharmacy component
Control
Pharmacy component
Control
Pharmacy component
Control
Pharmacy component
Control Cooney 201520 IG=1,070 CG=1,129
NR NR NR NR NR NR Classes of antihypertensives: P=.02 (subjects in IG prescribed more classes of anti-HTN
meds)
ESRD 26/1070 (2.4%)
ESRD 20/1129 (1.8%) P=.28
Aspinall 2012/201321,22 IG=314 CG=67 (Additional 91 patients receiving usual care at ESA clinic)
NR NR NR NR NR NR Medication adjustment based on
hemoglobina
Increased 176/305 (57.7%)
Withheld or Decreased
80/131 (61.1%)
Increased 30/105 (28.6%) (P=.009)
Withheld or Decreased
37/108 (34.3%) (P=.09)
Costb
$13,412
QALYs 2.096
Cost $16,173
QALYs 2.093
Pai 200918 IG=57 CG=47
NR NR NR NR Significantly (P=.02) fewer all-cause hospitalizations
in intervention group (overall 42% fewer hospitalizations in intervention group)
Mean number of drugs significantly (P<.05) lower
in intervention group at each medication review
(overall 14% fewer drugs in intervention group)
Mean drug costs were lower among patients in
intervention group; difference significant
(P<.05) only at 3rd drug therapy review (overall $6 less in intervention group)
Bucaloiu 200719 IG=62 CG=74
NR NR NR NR NR NR Weekly dose of EPO
6,698 units
12,000 units
(P=.001)
Estimated annual cost savings per patient
$3,860 CG = control group; EPO = epoetin alfa; ESA = erythropoiesis-stimulating agents; IG = intervention group; NR = not reported; QALYs = quality-adjusted life years a Proportion of hemoglobin tests resulting in change in ESA dose b Modeled over 5 years
Pharmacist-led Chronic Disease Management Evidence-based Synthesis Program
81
Table 10. Goal Attainment Outcomes – Chronic Kidney Disease Studies
Study; Intervention (n) Control (n)
Patient Goal Attainment definition Percentage of patients attaining goal (n/N)
Pharmacy component Control Cooney 201520 IG=1,070 CG=1,129
BP Control <130/80mmHg 185/441 (42.0%)a 177/429 (41.2%)a
(P=.84)
Aspinall 2012/201321,22 IG=314 CG=67 (Additional 91 patients receiving usual care at ESA clinic)
Hemoglobin 10-12g/dL Proportion of values within range 1284/1807 (71.1%)
Proportion of values within range 345/606 (56.9%)
(P<.001)
Bucaloiu 200719 IG=62 CG=74
Hemoglobin in goal range (11-12.9 mg/dL) Average iron saturation (T-sat) in goal range (20%-
50%)
69.8% of measured values
64.8% of measured values
43.9% of measured values (P=.0001)
40.4% of measured values (P=.043)
BP = blood pressure; CG = control group; IG = intervention group; NR = not reported a Denominators are patients with BP > 130/80mmHg at baseline
Pharmacist-led Chronic Disease Management Evidence-based Synthesis Program
82
Table 11. Study and Intervention Characteristics – Chronic Obstructive Pulmonary Disease Studies
Author, year Study design Type of Clinic
Target Population
Duration of study/
follow-up
Inclusion/ Exclusion Criteria
Goal of Intervention
Primary Outcome
Type of pharmacist Pharmacist Intervention Comparator
intervention Collaboration
Solomon 199823 Gourley 199824
RCT
10 VA Medical Centers; 1 University Hospital (8 sites participate in COPD trial)
Patients with COPD
6 months
Inclusion: -ambulatory COPD patient -pulmonary function tests for diagnosis -currently treated for COPD (≥1 inhaler) -capable of using inhaler -read & write English -≥40 years old -access to telephone Exclusion: -history of severe/life-threatening COPD -life-expectancy < 6 months -hospitalized or ED visit past 2 weeks -lung infection past 2 weeks -CHF class III or IV -other lung disease except asthma -alcohol or drug abuse -investigational drug trial within past 30 days
Improve compliance, patient satisfaction, knowledge, and quality of life
Patient knowledge, medication compliance, health resource use
Clinical pharmacists
N=43 Standardized patient assessment and a series of regularly scheduled therapeutic and educational interventions designed for optimal disease management -Implement care plan -Educate patients -Counsel patients -Patient assessment and follow-up Focused on management of COPD patients relative to: -Symptom control -Patient compliance -Drug product selection -Use of resources -Patient satisfaction with care -Disease and disease management -Knowledge -Quality of life
Mode/Frequency: -6-month treatment period with scheduled visits for treatment patients at enrollment and then at one-month intervals (4-6 wks) for a total of 5 visits -Telephone follow-up
N=55 Usual care (no supplemental education or assessment of needs beyond what was customarily offered at each site)
Collaborate with physicians to implement a patient-specific, optimized, step-care approach
CHF = congestive heart failure; COPD = chronic obstructive pulmonary disease; ED = emergency department
Pharmacist-led Chronic Disease Management Evidence-based Synthesis Program
83
Table 12. Drug-related Problems Outcomes – Chronic Obstructive Pulmonary Disease Studies
Study Intervention (n) Control (n)
Inappropriate dosage/prescription
or omission % (n/N)
Ineffectiveness% (n/N) Drug-drug or drug-disease interaction (describe) % (n/N)
Non-adherence to prescribed regimen
% (n/N) Clinical/adverse events % (n/N)
Pharmacy component Control Pharmacy
component Control Pharmacy component Control
Pharmacy component Control
Pharmacy component Control
Solomon 1998 Gourley 199823,24 IG=43 CG=55
Drug needed not prescribed 4.5%
(15/336 problems identified by pharmacists)
Drug not needed but prescribed 1.5% (5/336) Dose problem 1.2% (4/336)
NR NR NR Risk of interaction
8.9% (30/336 problems
identified by pharmacists)
NR NR NR NR NR
CG = control group; IG = intervention group; NR = not reported
Table 13. Mortality, Quality of Life, Access, and Patient Satisfaction Outcomes – Chronic Obstructive Pulmonary Disease Studies
Study; Intervention (n) Control (n)
All-cause mortality % (n/N)
Health-related quality of life (describe)
Access to care (describe)
Patient satisfaction with care (describe)
Pharmacy component Control Pharmacy
component Control Pharmacy component Control
Pharmacy component Control
Solomon 1998 Gourley 199823,24 IG=43 CG=55
NR NR Global Symptom Assessmenta
Baseline: 3.4 (1.1) 6 months: 3.2
(1.2) Quality of Lifeb (8
items) No significant changes from baseline; no
differences from control group
Baseline: 3.4 (1.3) 6 months: 3.3
(1.5)
Significant worsening of “bodily pain”
dimension from baseline to 6
months (P=.03)
NR NR PCQ – 10 items Intervention group patients
had more favorable response to pharmacist
than control for all 10 items; differences were significant
(P<.05) for 7 of 10 items
a Patient rating of overall status with respect to control of COPD: 0 = no symptoms present, 5 = symptoms so severe that one could not perform normal daily activities b Health Status Questionnaire 2.0 CG = control group; IG = intervention group; NR = not reported; PCQ = Pharmaceutical Care Questionnaire (developed for the study and addressing technical-professional competency, patient knowledge, and interpersonal relationship)
Pharmacist-led Chronic Disease Management Evidence-based Synthesis Program
84
Table 14. Healthcare Utilization and Cost Outcomes – Chronic Obstructive Pulmonary Disease Studies
Study; Intervention (n) Control (n)
Office visits Urgent care visits/
Emergency room (ER) visits
Hospitalizations Medications Costs or Other (describe)
Pharmacy component
Control
Pharmacy component
Control
Pharmacy component
Control Pharmacy
component Control
Pharmacy component
Control Solomon 1998 Gourley 199823,24 IG=43 CG=55
Mean (std) 0.81 (0.93)a
1.17 (1.03) (P<.05)
Mean (std) 0.15 (0.36)a
0.17 (0.48) (P=NS)
Mean (std) 0.10 (0.37)a
0.13 (0.34) (P=NS)
New medicationsa Mean (std) 0.51 (0.93)
0.36 (0.71) NR NR
a At 6 month follow-up CG = control group; IG = intervention group; NR = not reported; NS = not statistically significant
Table 15. Goal Attainment Outcomes – Chronic Obstructive Pulmonary Disease Studies
Study; Intervention (n) Control (n)
Patient Goal Attainment definition Percentage of patients attaining goal (n/N)
Pharmacy component Control No studies reporting
Pharmacist-led Chronic Disease Management Evidence-based Synthesis Program
85
Table 16. Study and Intervention Characteristics – Depression Studies
Author, year Study design Type of Clinic
Target Population
Duration of
study/ follow-up
Inclusion/ Exclusion Criteria
Goal of Intervention
Primary
Outcome
Type of pharmacist Pharmacist Intervention Comparator
intervention Collaboration
Adler, 200425 RCT Primary care clinics: 5 academic, 2 suburban, and 1 urban
Positive screen for depression or dysthymia 6 months
Inclusion: -met DSM-IV diagnostic criteria for major depressive disorder and dysthymia -no terminal illness, pregnancy, alcoholism, bipolar or psychotic disorder -English language literate -age ≥18 -patient consent
Increase antidepressant (AD) use AD use & changes in severity of depression as measured by a modified Beck Depression Inventory (mBDI)
Experienced clinical pharmacists with PharmD
N=258 -Medication history -Assess drug-related problems -Monitor drug efficacy & toxicity -Patient education & encouragement -Communicate findings to primary care provider -General social support, help overcoming system inadequacies, encourages patients, facilitates referrals Mode/Frequency: -At least 9 contacts in18 months -Initial contact by telephone to set up appointment
N=249 Standard Primary care physician (PCP) care
Information sharing with PCP
Capoccia, 200426 Boudreau, 200227 RCT University urban family practice
Referred to study after a new DSM-IV diagnosis of depression & Rx for AD 12 months
Inclusion: -no terminal illness, substance abuse, psychosis, pregnancy, suicide attempt; -English language -age ≥18 -patient consent
Improve outcomes Reduction in depression as measured by no longer meeting diagnostic criteria and improvement in symptom checklist (SCL-20)
Experienced staff clinical pharmacist and PharmD resident
N=41 -As many as 13 follow-up telephone calls to assess symptoms, concerns, and side effects; titrate doses; discontinue or change medication; manage Ads; patient education & motivation -Facilitated appointments with mental health -Additional therapy for other issues (ie sexual dysfunction/insomnia) -Provide support Mode/Frequency: -Weekly calls first 4 weeks, every 2 weeks through week 12, every other month from 4-12 months -Subjects encourage to visit PCP at weeks 4 and 12
N=33 Usual care (encouraged to use available resources which included pharmacists)
Primary care & psychiatrist case review with physicians
Pharmacist-led Chronic Disease Management Evidence-based Synthesis Program
86
Author, year Study design Type of Clinic
Target Population
Duration of
study/ follow-up
Inclusion/ Exclusion Criteria
Goal of Intervention
Primary
Outcome
Type of pharmacist Pharmacist Intervention Comparator
intervention Collaboration
Finley, 200328 RCT Urban primary care clinics of HMO
Primary care initiation of AD 6 months
Exclusion: -AD used in prior 6 months -concurrent psychiatric or psychological treatment -mania or bipolar disorder -psychotic symptoms -eminent suicidality -substance abuse or dependence -psychiatric treatment indicated
Improve drug adherence, patient outcomes, provider and patient satisfaction, and medical resource utilization Antidepressant adherence measured as medication possession ratio (MPR) & continued antidepressant between 3-6 months
Experienced clinical pharmacists with PharmD
N=75 -Intake interview: drug, medical, & psychiatric history; contraindications -Patient education: use of ADs, treatment options -Titration of ADs -Prescribe ancillary medications -Recommend changes in ADs -Follow-up for adherence, drug benefits and side effects, other social factors -Assess severity of condition -Identified stressors, other key factors Mode/Frequency: -Intake interview -5 follow-up contacts by phone and 2 clinic visits & on-call
N=50 Usual care - brief counseling on the prescribed drug, therapeutic end points, and side effects
Psychiatrist mentor met with clinical pharms to discuss and update on patients and consult Approval needed from PCP to change drug
Finley, 200229 Non-randomized comparison group; pilot study Urban primary care clinics of HMO
Primary care initiation of AD 6 months
Inclusion: -identified by PCP as suffering from depression -received prescription for AD medication Exclusion: -AD use past 6 months -under care of psychiatrist in HMO -imminent suicidality -psychotic symptoms -active substance abuse/dependence -history of manic episodes
Increase medication adherence and patient satisfaction Medication adherence rates, patient satisfaction, and resource utilization patterns
Experienced clinical pharmacists with PharmD and psychiatric experience
N=91 -Intake interview including: medication, medical, social, and mental health history; symptoms; and environmental stressors -Patient education including disease information, use of ADs, treatment options, importance of adherence, and potential adverse effects -Pharmacists could prescribe ancillary medications and recommend changes in ADs Mode/Frequency: -Intake interview -5 follow-up contacts by phone and 2 clinic visits & on-call
N=129 unmatched Usual care (treated by PCP)
Psychiatrist mentor, recommended medication changes to PCP
AD = antidepressant medication; DSM-IV = Diagnostic and Statistical Manual of Mental Disorders, 4th Edition; HMO = health maintenance organization; mBDI = modified Beck Depression Inventory; MPR = medication possession ratio; PCP = primary care provider; PharmD = Doctor of Pharmacy; RCT = randomized controlled trial; Rx = prescription; SCL-20 = Symptom Checklist Depression Scale
Pharmacist-led Chronic Disease Management Evidence-based Synthesis Program
87
Table 17. Drug-related Problems Outcomes – Depression Studies
Study Intervention (n) Control (n)
Inappropriate dosage/prescription
or omission % (n/N)
Ineffectiveness% (n/N) Drug-drug or drug-disease interaction (describe) % (n/N)
Non-adherence to prescribed regimen % (n/N)
Clinical/ adverse events % (n/N)
Pharmacy componen
t Control
Pharmacy componen
t Control
Pharmacy componen
t Control Pharmacy
component Control Pharmacy component Control
Capoccia 200426 IG=41 CG=33 3 outcome assessments over 12 months; extracted 12 month data
NR NR NR NR NR NR 12 months Patient reported use <25 of last
30 days 41%
Patient reported use <25 of last 30
days 43%
NR NR
Finley 200328 IG=75 CG=50
NR NR NR NR NR NR 3 month compliance
76%; MPR 0..92
6 month
compliance 67%;
MPR 0.83
3 month compliance
60%; MPR 0.89 (P=.48)
6 month
compliance 48%; MPR 0.77
(P=.26)
NR NR
Finley 200229 IG=91 CG=129
NR NR NR NR NR NR 6 month MPR 0.81
Use of ADs after 3 months
76%
6 month MPR 0.66
(P<.005)
Use of ADs after 3 months
51% (P=.001)
NR NR
AD = antidepressant medication; CG = control group; IG = intervention group; m=months; MPR = medication possession ratio; NR = not reported
Pharmacist-led Chronic Disease Management Evidence-based Synthesis Program
88
Table 18. Mortality, Quality of Life, Access, and Patient Satisfaction Outcomes – Depression Studies
Study; Intervention (n) Control (n)
All-cause mortality % (n/N)
Health-related quality of life (describe)
Access to care (describe)
Patient satisfaction with care (describe) Depression
Pharmacy
component
Control Pharmacy component Control Pharmacy
component Control Pharmacy component Control Pharmacy
component Control
Adler 200425 IG=258 CG=249
NR NR SF-12 Mental component (MCS)
40.4
Physical Component (PCS)
42.9
MCS 38.6 (P=.19)
PCS 42.9 (P=NS)
NR NR “Based on exit interviews patients expressed high
satisfaction with the pharmacist intervention”
NR NR
Capoccia 200426 IG=41 CG=33 3 outcome assessments over 12 months; extracted 12 month data
NR NR Mean SLC-20 NS difference (P=.92)
Mean SF-12 mental NS difference
(P=.46)
Mean SF-12 physical NS difference (P=.18)
NR NR Good or excellent quality of care (12 months):
80%
No overall difference in satisfaction
with depression
care (P=.19) or overall
healthcare (P=.48) between groups
Good or excellent quality of care: 77%
Diagnosis of major
depression: Groups similar (P=.32)
at 12
months at least 50% decrease in
SCL-20: 72%
at 12 months
at least 50% decrease in
SCL-20: 80%
(P=.39)
Pharmacist-led Chronic Disease Management Evidence-based Synthesis Program
89
Study; Intervention (n) Control (n)
All-cause mortality % (n/N)
Health-related quality of life (describe)
Access to care (describe)
Patient satisfaction with care (describe) Depression
Pharmacy
component
Control Pharmacy component Control Pharmacy
component Control Pharmacy component Control Pharmacy
component Control
Finley 200328 IG=75 CG=50
NR NR 56% reduction in WSDS (n=54)
67% reduction in
WSDS (n=24) (P=.36)
Mean of one 5-point
question about
availability of advice (higher=
more satisfied)
4.3 (n=59)
3.8 (n=33) (P<.05)
Mean of one 5-point question about treatment of depression, (higher= more satisfied) 4.2 (n=59) Significantly more satisfied with 6 out of 11 aspects of care (P<.05)
3.8 (n=33) Students t-test: P=.06 X2 test paired data: P=.066 Wilcoxon score: P=.023
41% with 50%
reduction in BIDS
Percent achieving remission
(BIDS score <9) 55.6%
(n=54)
54% with 50%
reduction in BIDS
(P=.27)
58.3% (n=24) (P=.36)
Finley 200229 IG=91 CG=129
NR NR NR NR Mean of one 5-point
question about
availability of advice (higher=
more satisfied)
4.3 (n=56)
3.7 (n=55) (P=.003)
Mean of one 5-point
question about
treatment of depression,
(higher= more
satisfied) 3.9 (n=56)
4.0 (n=59) (P=.581)
NR NR
AD = antidepressant medication; BIDS = Brief Inventory for Depressive Symptoms; CG = control group; IG = intervention group; NR = not reported; NS = not significant; SCL = symptom check list; SF-12 = Medical Outcomes Study Short Form 12; WSDS= Work and Social Disability Scale
Pharmacist-led Chronic Disease Management Evidence-based Synthesis Program
90
Table 19. Healthcare Utilization and Cost Outcomes – Depression Studies
Study; Intervention (n) Control (n)
Office visits Urgent care visits/
Emergency room (ER) visits
Hospitalizations Medications Costs or Other (describe)
Pharmacy componen
t Control
Pharmacy componen
t Control
Pharmacy componen
t Control
Pharmacy componen
t Control
Pharmacy componen
t Control Adler 200425 IG=258 CG=249
NR NR NR NR NR NR Patient on ADs
3 months: 61%
6 months: 58%
3 months: 49%
(P=.024) 6 months:
46% (P=.025)
NR NR
Capoccia 200426 IG=41 CG=33 3 outcome assessments over 12 months; extracted 12 month data Median(range)
All provider visits:
median 9 range
(0 to 42)
Visits to PCP
median 4 range
(0 to 21)
median 9 range
(0 to 60) (P=.99)
median 5 range
(0 to 17) (P=.88)
median 0 range
(0 to 2)
median 0 range
(0 to 2) (P=.27)
NR NR NR NR NR NR
Finley 200328 IG=75 CG=50
PCP visits decreased
15%
increased 2%
(P=.14)
Increased 7%
Increased 119%
(P=.10)
NR NR Changed ADs 19% (14/75)
4% (2/50) (P=.016)
Drug cost 42% higher
(P=.18)
Finley 200229 IG=91 CG=129
To PCP decreased 39% (335
to 203)
decreased 12% (411
to 361) difference between changes (P=.007)
NR NR NR NR Changed ADs 24%
(22/91)
5% (7/129) (P=.001)
NR NR
AD = antidepressant medication; CG = control group; IG = intervention group; NR = not reported; PCP = primary care provider
Pharmacist-led Chronic Disease Management Evidence-based Synthesis Program
91
Table 20. Goal Attainment Outcomes – Depression Studies
Study; Intervention (n) Control (n)
Patient Goal Attainment definition Percentage of patients attaining goal (n/N)
Pharmacy component Control No studies reporting
CG = control group; IG = intervention group; NR = not reported
Pharmacist-led Chronic Disease Management Evidence-based Synthesis Program
92
Table 21. Study and Intervention Characteristics – Diabetes Studies
Author, year Study design Type of Clinic
Target Population
Duration of
Study/ Follow-up
Inclusion/Exclusion Criteria
Goal of Intervention
Primary
Outcome
Type of Pharmacist Pharmacist Intervention Comparator
Intervention Collaboration
McAdam-Marx 201553 Retro-spective cohort University-owned community-based primary care clinics
Patients with inadequately controlled T2DM (HbA1c<7%) Follow-up: max of18 months
Inclusion: -Intervention group: patients referred to diabetes collaborative care management (DCCM) by PCP; age ≥ 18; T2DM; treated at community clinic offering DCCM; treated ≥180 days prior to index date; follow-up care in clinic 3 to 18 months after index date -Control group: adults with T2DM treated at clinic without DCCM Exclusion: -HbA1c <7%
Improve patient outcomes Glycemic control (HbA1c) during 18 months post-index date
Clinical pharmacist
N=303 -Pharmacists able to prescribe and modify diabetes medication therapy, adjust insulin dosing, order HbA1c and lipid monitoring tests, and provide diabetes education - Follow-up visits included dose adjustments, adherence and disease education, and addressing patient questions Mode/Frequency: Initial in-person visit then telephone and in-person visits every 1-2 weeks until goals met or patient no longer engaged in program
N=394 Usual care
Referred to DCCM program by PCP; pharmacists worked under collaborative practice agreement with physicians and advanced practice clinicians
Skinner 201535 Retro-spective case-control Community health clinic
Uncontrolled diabetes 12-month study period
Inclusion: -age ≥ 18 -diabetes diagnosis -≥1 documented HbA1c>7% -a risk factor for disease-related microvascular complications -referred to MTM by PCP -clinical data from at least 3 clinic visits during a consecutive 12m period
Improve medication adherence and diabetes health outcomes
Clinical pharmacist
N=29 Medication Therapy Management -pharmacist reviewed patient’s T2DM medication regimen -verbal education and training on medication delivery and best administration sites -education on health-promoting behaviors -patients asked to teach back the information to confirm understanding Mode/Frequency: mode not reported; frequency data not collected
N=29 (Matched sample – age, gender, race, ethnicity, BMI) -Usual care/no contact with clinical pharmacist
Referred to pharmacist for MTM by PCP
Pharmacist-led Chronic Disease Management Evidence-based Synthesis Program
93
Author, year Study design Type of Clinic
Target Population
Duration of
Study/ Follow-up
Inclusion/Exclusion Criteria
Goal of Intervention
Primary
Outcome
Type of Pharmacist Pharmacist Intervention Comparator
Intervention Collaboration
Chung 201450 Retro-spective review via EMR CommUnity Care, outpatient clinics in Austin
Type1 or 2 diabetes mellitus 4-year study period 1 year follow-up for each patient
Inclusion: -age 18-89 -diagnosis of T1 or 2 DM -documentation of HbA1c ≥9% at baseline (3 months before or after index visit) -≥ 3 visits with clinical pharmacist or usual care provider -eligible for ≥ 1 yr before and after index dates -documented follow-up HbA1c Exclusion: -clinical pharmacy visit for any disease state before study initiation -diagnosis of cancer or HIV -pregnant -diagnosis code for motor vehicle accident or chronic pain
Assess the effect of clinical pharmacist involvement in a federally qualified health center on the change in A1c and frequency of diabetes related hospitalizations and ED visits 1 year post index change in A1c, diabetes-related hospitalizations, diabetes-related ED visits
Pharmacists who have completed at least 1 year of a postdoctoral residency training program
N=225 (matched N=220) -Implementing new medications -Titrating medications -Ordering laboratory panels -Counseling on lifestyle modification -Providing diabetes education -Managing associated comorbid conditions Mode/Frequency: -30 minute visit as often as needed or necessary to meet goals and/or for patient safety
N=557 (matched N=220) Usual care, followed by PCP and no appointments with a clinical pharmacist during study period
None mentioned
Pharmacist-led Chronic Disease Management Evidence-based Synthesis Program
94
Author, year Study design Type of Clinic
Target Population
Duration of
Study/ Follow-up
Inclusion/Exclusion Criteria
Goal of Intervention
Primary
Outcome
Type of Pharmacist Pharmacist Intervention Comparator
Intervention Collaboration
Spence 201413 Retro-spective cohort Kaiser Permanent Southern California (KPSC) Region – outpatient pharmacy service
Non-adherent diabetes mellitus patients with HbA1c outside clinical goals 1 year after index date
Inclusion: -in KPSC’s diabetes registry -non-adherent (Medication Possession Ratio <0.8) -on ≥1 oral medication for DM -at or above the HbA1c target of 8% -age >18 -enrolled with a pharmacy benefit for ≥1 year before and after index date Excluded: -active insulin prescription -resided in skilled nursing facility for >10 days or had received hospice care -OPCS patients that declined the consult
Improve medication adherence and likelihood of achieving clinical goals Not specified
Pharmacists participated in 5.5 hours of online and face to face training
N=359 Outpatient pharmacy clinical service (OPCS) program -B-SMART medication optimization process (identify barriers and assess readiness to change, provide solutions to adherence challenges, motivation, adherence tools, identify roles of health care team members, direct patients to other resources) -Pharmacist consult at time of prescription pick-up -Printing of a care management summary sheet -Spontaneous identification of non-adherent patients at the time the patient arrives at the pharmacy Mode/Frequency: -Face-to-face -One time (at prescription pick-up)
N=428 matched Did not receive an OPCS consultation
None noted
Brummel 201346 Non-randomized controlled trial Fairview Pharmacy Services, MN, Healthcare system
Diabetes 1 year of intervention and 1 year follow-up
Inclusion: -attended one of the clinics and decided to opt in to MTM program -all information on medications was available at baseline and all outcome measures were available for 2006, 2007, and 2008 -Control – those who didn’t opt in to MTM program
Identify and resolve drug therapy problems and promote optimal patient outcomes Achieving optimal diabetes clinical management, determined with 5 component diabetes measure (D5)
MTM pharmacist
N=121 -Provided consultations using validated, standardized process -Pharmacists’ responsibilities included assessing patient’s medications, identification of patient’s drug-related needs, resolution and prevention of drug-related problems, determining appropriate follow-up measures, and documentation of intervention outcomes -Initiate, modify, or discontinue drug therapy and order laboratory tests related to diabetes, hypertensions, and hyperlipidemia Mode/Frequency: -Primarily face-to-face
N=103 Usual care, not in MTM program
None mentioned
Pharmacist-led Chronic Disease Management Evidence-based Synthesis Program
95
Author, year Study design Type of Clinic
Target Population
Duration of
Study/ Follow-up
Inclusion/Exclusion Criteria
Goal of Intervention
Primary
Outcome
Type of Pharmacist Pharmacist Intervention Comparator
Intervention Collaboration
Ip 201343 Dual-centered retro-spective study 2 Kaiser Permanente (KP) medical centers
Type 2 diabetes 12 months
Inclusion: -HbA1c >7% -type 2 diabetes -age > 18 -under the pharmacist’s care for ≥ 2 months Exclusion: -type 1 diabetes -HbA1c<7% -patients who dis-enrolled from KP health insurance during the study time frame
Investigate the impact of pharmacist interventions on short-term clinical markers and long-term cardiovascular risk Change in HbA1c, LDL-C, & BP; rates of goal attainment; and change in predicted 10yr risk of coronary heart disease/stroke
Credentialed as certified diabetes educator and pharmacotherapy specialist
N=147 -Initial in-person visit with follow-up until therapeutic goals were met -Evaluated diabetes status and CV comorbidities -Pharmacotherapy modifications (prescribing and dosage adjustments) -Laboratory monitoring -Dietary and physical activity recommendations -Provision of diabetes self-care education -Physical assessments -Immunizations -Specialist referrals -Followed up for further care Mode/Frequency: -45-min face-to-face initial visit with follow-up in person or via telephone
N=147 PCP care (no pharmacist visit)
Referred by and discharged from program to PCP
Pharmacist-led Chronic Disease Management Evidence-based Synthesis Program
96
Author, year Study design Type of Clinic
Target Population
Duration of
Study/ Follow-up
Inclusion/Exclusion Criteria
Goal of Intervention
Primary
Outcome
Type of Pharmacist Pharmacist Intervention Comparator
Intervention Collaboration
Heisler 2010/20123
3,34 cRCT effectiveness study (team clusters randomized then patient randomized within team) 3 VA (2 academically affiliated) 2 KP facilities, primary care teams
Diabetes 14-month intervention period, patient discharged when adherence issues were addressed, BP was at target, statin was prescribed if indicated, and glycemic control addressed. Patients received a median of 9 weeks follow-up. Data also collected for the 6 months prior to and after the intervention period
Inclusion: In last 12 months -1 hospitalization or 2 outpatient visits with diabetes related code or ≥1 prescription for diabetes medication -most recent SBP≥140 and mean SBP (last 9 months) >140 or most recent SBP ≥150 and no other BP measures for last 9 months -poor refill adherence (gaps totaling ≥20% of days supply of ≥1 BP medication over prior year or insufficient medication intensification within 30 days prior to or any time after last BP (increase in number drug classes, daily dosage, or switch to another medication)) Exclusion: -pregnant -age < 18 or > 100 -impaired decision-making -KP patients excluded if on “no contact” list, hospitalized, nursing home resident, hospice or home health care; < 12 months of active drug benefit
BP control Relative change in systolic BP
Clinical pharmacist, trained in motivational interviewing and authorized to adjust BP and lipid medications
8 teams, N=2,319 with 1,797 activated -Proactive case identification using medication management tool database -Pharmacists referred to database which assisted in tracking and scheduling patient encounters and assessing adherence -Adherence counseling and assessment -Medication management -Recent clinical indicators discussed -Labs ordered -Medication changes could be made -Patients made/discussed goals -Pharmacist constructed specific, short-term action plan Mode/Frequency: -In-person or by telephone -Continued until patient was discharged from intervention program
8 teams, N=2,303 Usual care enhanced by information given to providers about patients’ adherence and intensification problems; access to care manager and non-study clinical pharmacy services All patients; in-person or telephone intake by pharmacist plus welcome packet with educational materials
Copied provider on all clinical notes; alerted PCP when patient declined program, entered program or was discharged from program; pharmacists required to consult with PCP if patient was on 3 anti-hypertensives
Pharmacist-led Chronic Disease Management Evidence-based Synthesis Program
97
Author, year Study design Type of Clinic
Target Population
Duration of
Study/ Follow-up
Inclusion/Exclusion Criteria
Goal of Intervention
Primary
Outcome
Type of Pharmacist Pharmacist Intervention Comparator
Intervention Collaboration
Jacobs 201238 RCT Ambulatory general internal medicine setting (Lahey clinic) in Burlington, MA
Type 2 diabetes 1 year
Inclusion: -age > 18 -documented HbA1c > 8% obtained more than 6 months earlier Exclusion: -receive primary care outside of Lahey Clinic Burlington campus -type 1 diabetes -HbA1c < 8% within 6 months -enrolled in another pharmacy or diabetes study -diabetes management by an outside endocrinologist -unable to adhere to study schedule
Improve glucose, lipid, and blood pressure control Achieving targets for HbA1c, LDL cholesterol, and blood pressure
5 clinical pharmacist practitioners who had PharmD degrees and minimum of post-graduate residency training with emphasis on ambulatory care practice with direct care for patients with chronic disease
N=72 Pharmacist visit included: -comprehensive medication review -targeted physical assessment -education on diabetes pathophysiology and importance of control -ordering laboratory tests -reviewing, modifying, and monitoring patients’ medication therapy -detailed counseling on all therapies -facilitating self-monitoring of blood glucose -providing reinforcement of dietary guidelines and exercise -facilitate referrals to other clinicians Mode/Frequency: -Required to attend at least 3 clinic visits with pharmacist (baseline, 6 and 12 months)
N=92 Usual care as directed by physician according to current standard of practice
Therapy, monitoring, and referral recommenda-tions required approval by the patient’s physician
Pharmacist-led Chronic Disease Management Evidence-based Synthesis Program
98
Author, year Study design Type of Clinic
Target Population
Duration of
Study/ Follow-up
Inclusion/Exclusion Criteria
Goal of Intervention
Primary
Outcome
Type of Pharmacist Pharmacist Intervention Comparator
Intervention Collaboration
Salvo 201249 Retro-spective cohort County-funded health center, St. Louis
“Indigent” (low-income, minority) with diabetes (1 or 2) using insulin 2-year time frame
Inclusion -using insulin -ambulatory -speak English -age 18-64 -diabetes diagnosis Exclusion: -seeing an endocrinologist -from standard care if had current or previous interactions regarding diabetes management with pharmacy team
Glycemic control and preventive care measures Change in HbA1c between groups between baseline and various end points
Board-certified residency-trained pharmacist, full-time faculty member of the St. Louis College of Pharmacy and pharmacy resident and students
N=69 Pharmacist-managed insulin titration program -Initially meeting: discuss diabetes management, role of preventive care measures, self-monitored blood glucose, complications, and pharmacist program -Review medical record to determine need for medication initiation, adjustment or discontinuation, lab monitoring, and preventive care measures -Follow-up (telephone) every 1-2 weeks: patient reports insulin regimen, self-monitored blood glucose, adverse events. -Assess adherence, educate on lifestyle modifications and medication adherence, adjust insulin dosage -Preventive care assessment at each interaction -Schedule appointments with specialists (podiatrist, dietician) Mode/Frequency: -Initial in-person meeting then telephone follow-up every 1-2 weeks
N=57 matched Standard care
Pharmacist notifies PCP of insulin adjustments and reminds of overdue lab work/vaccines
Pharmacist-led Chronic Disease Management Evidence-based Synthesis Program
99
Author, year Study design Type of Clinic
Target Population
Duration of
Study/ Follow-up
Inclusion/Exclusion Criteria
Goal of Intervention
Primary
Outcome
Type of Pharmacist Pharmacist Intervention Comparator
Intervention Collaboration
Cohen 201132 RCT (VA-MEDIC-E) Primary care, VA, urban (Providence)
Type 2 diabetes 6 months
Inclusion: -type 2 diabetes -HbA1c>7%; LDL>100mg/dL or >70mg/dL if CAD; BP>130/80 mmHg (each documented in last 6 months) -willing to discuss diabetes and cardiac risk factors in group setting Exclusion: -gestational diabetes -unable to attend sessions -condition precluding diabetes self-care
CV Risk Reduction Primary Outcome: change in proportion of participants achieving target glycemic and cardiac risk factor goals
Clinical pharmacist, trained in diabetes education with prescribing privileges
N=50 Regular visits with PCP plus -Education -Behavioral and pharmacologic interventions for hypertension, hyperlipidemia, hyperglycemia, and tobacco use -Received CV report card and exercise prescription, set diet and activity goals -Medication regimens discussed and evaluated, doses titrated -Referrals Mode/Frequency: -4 once-weekly 2-hour educational sessions (1 hour education, 1 hour behavioral and pharmacologic interventions) -5 monthly booster sessions
N=49 Standard Primary care, average. once every 4 months, 20-60 minute appointments, may include referrals
Education session provided by pharmacist, dietitian, nurse and physical therapist -also saw PCP
Padiyara 201145 Retro-spective EMR review Primary care clinic affiliated with multi-specialty medical group; suburban metropolitan area
Diagnosed with diabetes mellitus 1 year
Inclusion -age ≥18 -2 or more visits with the pharmacist-managed diabetes clinic during study period (control group had at least 2 PCP visits and no pharmacist clinic visits)
Educate and directly manage drug therapy and preventive care services
3 university-affiliated pharmacists
N=321 -Emphasized the ADA guidelines -Pharmacists have autonomy in: -assessing patients -providing disease-state education -reviewing current medication lists -initiating or adjusting medication therapy -ordering laboratory tests -determining appropriate follow-up
Mode/Frequency -45-minute initial meeting; 30-minute visits for returning patients; had at least 2 pharmacist or PCP visits to be included in study
N=321 randomly selected Usual care includes provision of preventive care services and screenings; medication management; education of patient by PCP, or other staff; and referral to other specialist if appropriate
Some patients referred to pharmacist clinic by PCP
Pharmacist-led Chronic Disease Management Evidence-based Synthesis Program
100
Author, year Study design Type of Clinic
Target Population
Duration of
Study/ Follow-up
Inclusion/Exclusion Criteria
Goal of Intervention
Primary
Outcome
Type of Pharmacist Pharmacist Intervention Comparator
Intervention Collaboration
Pape 201148 Prospective cRCT (clinics randomized) Providence Primary Care Research Network, internal medicine/ family practice clinics (Oregon)
Diabetes Inclusion: -problem list entry of diabetes on EMR -age ≥ 18 Exclusion: -no evidence of medical chart activity within 3 years
Cholesterol management in diabetes Proportion of participants in each arm achieving a target LDL-C level < 100mg/dL
Clinical pharmacists
6 clinics, N=4,160 Health IT resources plus -Reviewed medical charts of patients with elevated LDL-C level -Developed individualized, evidence-based treatment recommendations to include medication therapy and follow-up laboratory monitoring -Treatment plan sent to PCP for review -Physician could ignore recommendation, act on it or approve intervention by pharmacist Mode/Frequency: -If intervention approved: pharmacist contacted patient by phone, education provided to support a shared decision-making process for treatment plan
3 clinics, N=2,069 Clinics randomized to control had access to CareManager disease management software which provided automated quality reporting, benchmarking, and robust care opportunity decision support
Treatment plan shared with PCP who could decide how to react Pharmacist supported by medical assistant who triaged lab results, ordered overdue labs, scheduled appointments, and facilitated mailings (by protocol)
Pharmacist-led Chronic Disease Management Evidence-based Synthesis Program
101
Author, year Study design Type of Clinic
Target Population
Duration of
Study/ Follow-up
Inclusion/Exclusion Criteria
Goal of Intervention
Primary
Outcome
Type of Pharmacist Pharmacist Intervention Comparator
Intervention Collaboration
Taveira30 2011 RCT (VA-MEDIC-D) Providence VA Medical Center
Type 1 or Type 2 diabetes AND depression 6 months
Inclusion: -type 1 or 2 diabetes -age ≥ 18 -HbA1c >6.5% within last 6 months -concomitant depression -willing to discuss diabetes and cardiovascular risk factors in group setting Exclusion: -gestational DM -unable to attend group session -disease condition, psychiatric instability, or organic brain injury precluding diabetes self-care
Management of diabetes and CV risk factors Change in proportion of participants who attained a goal HbA1c of <7% at 6 months
Clinical pharmacist with prescribing authority and certified diabetes educator
N=44 -Regular visits with PDP and standard visits with mental health provider -Education part of session: interactive lectures presented by a nurse, nutritionist, or clinical pharmacists, focused on self-care behaviors (eg, goal setting, promoting healthy problem solving) -Food logs reviewed by pharmacist and participants reminded of nutritional goals -Pharmacological and Behavioral intervention: conducted by clinical pharmacist, group assessment to determine degree to which patients felt they could manage their diabetes care daily, group counseling, reinforcement to enhance self-efficacy -Participants provided with CV risk report cards with medical history, medications, vitals, and laboratory values, reviewed during week 1 session, updated regularly -Medications titrated and initiated (no changes to psychiatric medications) -Individualized homework for medication changes and behavior change goals Mode/Frequency: -4 once-weekly sessions of 2 hours, then 5 monthly booster sessions held in classroom with 4-6 participants
N=44 -regular visits with primary care provider, approximately 30 minutes -referral to Diabetes Self-management Education Program (4 weekly education visits and monthly 90 minute follow-up appointments) -continue standard care with mental health providers
Education part of session presented by nurse or nutritionist too
Pharmacist-led Chronic Disease Management Evidence-based Synthesis Program
102
Author, year Study design Type of Clinic
Target Population
Duration of
Study/ Follow-up
Inclusion/Exclusion Criteria
Goal of Intervention
Primary
Outcome
Type of Pharmacist Pharmacist Intervention Comparator
Intervention Collaboration
Jameson 201036 RCT Community based primary care group (Advantage Health Physician Network) 13 offices, 3 urban, 9 suburban 1 rural
Diabetes 12 months
Inclusion: -age ≥18 -HbA1c ≥9% or no office visit within 12 months Exclusion: -being seen by an endocrinologist -not expected to live for duration of study
Improved management Change in HbA1c after 1 year
Board-certified pharmaco-therapy specialist with diabetes management and education training
N=52 Targeted patient outreach plus -assessment of adherence, barriers to optimizing blood glucose levels, and medication regimen -individualized education on self-management (diet, exercise, blood glucose level testing, medications, insulin) -followed guidelines of the Management of Type 2 Diabetes, including changing medication Mode/Frequency: -Initial home visit with study nurse to determine eligibility -In-person session with pharmacist at primary care site -Follow-up visits supplemented with phone calls
N=51 Usual care including registries to identify and track patients and targeted patient outreach
PCP approved any changes in medication or therapy
Johnson 201042 Retro-spective chart review “safety net” clinic medical homes, major urban city
Uninsured or underinsured with type 2 diabetes 2 years (mean 1.2 years for intervention group; 1.4 years for control group)
Inclusion: -HbA1c >9% -had a clinic visit during enrollment period -Age > 18 -second visit with HbA1c within 2 years of index visit -for intervention group: referred to pharmacist by usual provider
Disease management Change in A1c from baseline to last measured post-treatment A1c and whether or not the patient achieved the treatment goal of a final A1c<7%
Clinical pharmacist
N=222 -Reviewing medical, laboratory, and medication histories -Evaluating and modifying drug therapy under an established protocol -Ordering routine laboratory tests (HbA1c, lipid panel, metabolic panel, renal and liver function) -Monitoring adherence to drug therapy regimens -Educating patients -Providing follow-up care Mode/Frequency: -At least 2 clinic visits with laboratory value measurements
N=262 not matched Usual care no pharmacist
Referred by PCP
Pharmacist-led Chronic Disease Management Evidence-based Synthesis Program
103
Author, year Study design Type of Clinic
Target Population
Duration of
Study/ Follow-up
Inclusion/Exclusion Criteria
Goal of Intervention
Primary
Outcome
Type of Pharmacist Pharmacist Intervention Comparator
Intervention Collaboration
Taveira 201031 RCT (VA-MEDIC) Providence VA Medical Center
Type 2 diabetes 1 month-long intervention, follow-up at 4 months (3 months post)
Inclusion: -type 2 diabetes -age ≥18 -HbA1c 7% to 9% within previous 6 months -Willing to discuss diabetes and cardiovascular risk factors in group settings Exclusion: -unable to attend group settings -disease condition precluding diabetes self-care
Reduce cardiac risk factors Improve achievement of target goals in hypertension, hyperglycemia, hyperlipidemia, and tobacco use
Clinical pharmacists with prescriptive authority; certified in diabetes education and physical assessment with 6 months supervised pharmacy management
N=58 Regular PCP appointments plus -educational part of session: interactive lectures provided by nurse, nutritionist, physical therapist, or clinical pharmacist focused on diabetes self-care behaviors -behavior and pharmacological portion of session with clinical pharmacist: discussed and titrated medication regimens based on algorithms, wrote down medication changes, help with tobacco cessation, patients taught to carry CV risk report cards (see above) Mode/Frequency: -4 weekly, 2-hr sessions in a classroom setting with approximately 4-8 participants
N=51 Saw primary care provider at VA medical center through individual clinic visits, average frequency 4 months
Educational sessions also provided by nurse, nutritionist, and physical therapist
Fox 200947 Non-equivalent group, quasi-experimental study Florida Healthcare Plans HMO
Diabetes and Medicare part D, MTM eligible (≥ 3 chronic diseases and ≥ 4 maintenance medication and likely Part D medication costs ≥ $4000/year 1 year
Inclusion: -Medicare Part D member -eligible for comprehensive diabetes care (CDC) according to HEDIS -MTM eligible (3 or more chronic diseases and 4 or more maintenance medications and likely to have Medicare part D costs of >$4,000/yr) and chose to participate
Improve HEDIS LDL-C quality measures for CDC Presence of LDL-C screening, LDL-C values, and LCL-C control
Staff clinical pharmacists
N=255 -Medication therapy review and evaluation, sent to PCP; included: -drug-drug and drug-disease interactions -OTC drug therapy -medication monitoring, recommending changes if indicated -adherence to HEDIS comprehensive diabetes care guidelines and goals (LDL-C control and HbA1c, BP, and weight) -medication cost reduction -adherence counseling -adverse events, education -medication optimization, reducing cost and consolidating (not limited to lipid-lowering medications)
Mode/Frequency: -Telephone interview with pharmacist and follow-up calls if recommendations made (at least 3 calls)
Usual care – 2 groups 1) N=56 who did not participate in MTM 2) N=1,803 enrollees not eligible for MTM
Recommenda-tions shared with physician
Pharmacist-led Chronic Disease Management Evidence-based Synthesis Program
104
Author, year Study design Type of Clinic
Target Population
Duration of
Study/ Follow-up
Inclusion/Exclusion Criteria
Goal of Intervention
Primary
Outcome
Type of Pharmacist Pharmacist Intervention Comparator
Intervention Collaboration
Scott 200640 RCT Siouxland Community Health Center in Sioux City, Iowa
Type 2 diabetes Intervention for 3 months, total of 9 month follow-up
Inclusion: -SCHC members -age >18 -diagnosis of type 2 diabetes -referred by PCP Exclusion: -patient foresaw difficulty completing the study -migrant worker -drug abuse
Manage patients’ diabetes Reduction of HbA1c levels
Clinical pharmacist with 1 year primary care residency program
N=76 -Appointments focused on disease management, lifestyle adjustments, and goal setting -Group sessions: reviewed nutrition and basic diabetes management (nurse and dietitian participated) -pharmacist provided other therapeutic interventions (eg, aspirin therapy, influenza vaccine) and reminded patients about appointments Mode/Frequency: -Appointments every 2 weeks -Group-session appointments and telephone follow-up when necessary
N=73 Standard diabetes care, managed by a nurse All patients had appointments at baseline and 3, 6, & 9 months; incentive package for attending study appointments
Group appointments involved a pharmacist, dietitian, and nurse; medication change recommendations were given to provider and implemented by provider or pharmacist
Odegard 200551 RCT University of WA neighbor-hood primary care clinics, greater Seattle area
Type 2 diabetes 6 month intervention plus 6 month follow-up after intervention ended
Inclusion: -age ≥ 18 -type 2 diabetes -taking at least one oral diabetes medication -HbA1c ≥9% Exclusion: -non-English speaking -unstable psychiatric condition -terminal prognosis (within 6 months)
Improving diabetes control HbA1c levels
Primary care pharmacist
N=43 -Development of a diabetes care plan -Regular pharmacist-patient communication on diabetes care progress -Pharmacist-provider communication on diabetes care progress -Medication-related problems requiring intervention identified Mode/Frequency: -Initial in-person appointment then weekly in-person or telephone contact (decreased to monthly once care needs were progressing)
N=34 Baseline interview and continue normal care with PCP
Diabetes care plan was communicated to PCP through EMR notation, communication between pharmacist and PCP
Pharmacist-led Chronic Disease Management Evidence-based Synthesis Program
105
Author, year Study design Type of Clinic
Target Population
Duration of
Study/ Follow-up
Inclusion/Exclusion Criteria
Goal of Intervention
Primary
Outcome
Type of Pharmacist Pharmacist Intervention Comparator
Intervention Collaboration
Rothman 200539 cRCT (clinics matched and randomized) University of NC General Internal Medicine Practice
Vulnerable patients with poorly controlled type 2 diabetes February 2001 to April 2003, patients followed for 1 year
Inclusion: -age ≥ 18 -diagnosed with type 2 diabetes -followed for diabetes care in the practice -referred by provider -poor glucose control (HbA1c≥8%) -spoke English -life expectancy >6 months
Improve cardiovascular risk factors and HbA1c levels Blood pressure, A1c levels, cholesterol level, and aspirin use
Clinical pharmacist who could initiate and increase use of blood pressure-, cholesterol-, and glucose- lowering medications
N=105 Usual care plus -Management session: diabetes education, treatment recommendations to PCP -Intensive education sessions, counseling -Medication management -Evidence-based algorithms to initiate and increase use of blood pressure, cholesterol, and glucose lowering medications -Proactive management of clinical parameters -Diabetes care coordinator to address issues related to health behavior and education, remind of appointments, and help address barriers to care Mode/Frequency: -1 hour management session -Dedicated clinical slots for intervention group patients -Pharmacist contacted patients at least every 2-4 weeks
N=112 Management session plus usual care from PCP
Results from sessions with pharmacists shared with PCP Medication adjustments approved (before or after as requested by PCP)
Pharmacist-led Chronic Disease Management Evidence-based Synthesis Program
106
Author, year Study design Type of Clinic
Target Population
Duration of
Study/ Follow-up
Inclusion/Exclusion Criteria
Goal of Intervention
Primary
Outcome
Type of Pharmacist Pharmacist Intervention Comparator
Intervention Collaboration
Shane-McWhorter 200541 Retro-spective review Community health center, Utah; clinical pharmacy demonstra-tion project
Diabetes Charts were reviewed for all patients who received diabetes education from August 2000-June 2002 Outcomes collected over 1-3 years
Inclusion: -received at least one education session (IG) -diabetes
Enhancing patient care in the area of drug therapy and disease management No primary outcome specified
College of Pharmacy faculty clinician, certified diabetes educator
N=176 -Initial chart review: assess drug therapy, need for test/monitoring, health care maintenance needs, establish plan of action/education plan, evaluate appropriateness of drug therapies to look for potential interactions/adverse reactions -In-person patient education regarding diabetes, hypertension, hyperlipidemia, drug therapy, lifestyle modifications, ADA as components of self-management education -Individualized recommendations regarding drug therapy, lab testing, and healthcare maintenance -Obtained a detailed medical and drug therapy history -Needs assessment -Recommendations for provider regarding maintaining, changing, or adding drugs, certain tests, health care maintenance (made in chart note) -Follow-up education to document changes made by patient in nutrition or exercise, provide drug therapy education, information about health care maintenance and complications, determine if any tests still required -Chart reviews on continuing basis to track outcomes and provide recommendations Mode/Frequency: -In person -Monitoring 3 times/year (chart review)
N=176 randomly selected Access to a non-pharmacist health educator
Made recommenda-tions to physician
Pharmacist-led Chronic Disease Management Evidence-based Synthesis Program
107
Author, year Study design Type of Clinic
Target Population
Duration of
Study/ Follow-up
Inclusion/Exclusion Criteria
Goal of Intervention
Primary
Outcome
Type of Pharmacist Pharmacist Intervention Comparator
Intervention Collaboration
Stroup 200352 RCT The Endocrine Group, Albany NY, associated with the Albany College of Pharmacy
Poorly controlled diabetes mellitus 2 years
Inclusion: -patient at The Endocrine Group -minimum 1 year duration of HbA1c values greater than 10% -physician approved
Improve glycemic control Average HbA1c values over a 2yr period
2 consecutive groups of 6 fourth-year pharmacy students who had completed a 1-semester didactic program and shadowed a faculty member or more experienced student
N=30 -Students reviewed with each patient: -compliance with therapies -side effects, recent ED visits or hospitalizations -blood glucose monitoring -blood sugar logs -hypoglycemic management including insulin therapy and dosage adjustment -goals of therapy -diabetes complications -patient-initiated questions -diet, exercise, and weight loss
-Notes from visit were typed and delivered to endocrinologist and submitted into EMR Mode/Frequency: -Monthly hour-long visits in patients’ home
N=40 See physician as typically scheduled (every 3-4 months)
Acute problems immediately communicated verbally to patients’ endocrinolo-gists; notes from visit delivered to endocrinologist
Kelly 200044 CCT Richmond Health Care Group, a managed care-affiliated physicians group in Virginia
Diabetes 9 months
Inclusion: -diabetic patients taking oral diabetic agents or insulin -chosen by their providers to participate -documented HbA1c >8%, systolic >130mm Hg or diastolic >85mmHg, or LDL-c >120% of goal
Achieving near normoglycemia, lowering blood pressure, and LDL <130 mg/dL in patients with 2 or more CV risk factors or <100 mg/dL for patients with established disease HbA1c, SBP,DBP, and smoking cessation
Clinical site included one full-time clinical pharmacist/ faculty member, one pharmacy resident, and fourth-year Doctor of Pharmacy students
N=32 -Assessment/consultation on diabetes self-management -Complete medical history -Laboratory tests -Develop management plan, create short- and long-term goals, assess medication issues, and review nutrition recommendations, lifestyle changes, and blood-glucose monitoring instructions -Follow-up: reviewed goals, self-management plan, medications, hypoglycemic events, test results and lifestyle changes -Continuing education on self-management topics Mode/Frequency: -One-on-one assessment/consultation -Follow-up scheduled based on degree of monitoring required (usually monthly)
N=16 matched Historical controls, one year prior to implementation of clinical service
Dosage adjustments made in collaboration with PCP
Pharmacist-led Chronic Disease Management Evidence-based Synthesis Program
108
Author, year Study design Type of Clinic
Target Population
Duration of
Study/ Follow-up
Inclusion/Exclusion Criteria
Goal of Intervention
Primary
Outcome
Type of Pharmacist Pharmacist Intervention Comparator
Intervention Collaboration
Jaber 199637 RCT University-affiliated internal medicine outpatient clinic, urban, Detroit
Urban African-Americans with non-insulin-dependent diabetes mellitus (NIDDM) 4 months
Inclusion: -urban African-American patients -NIDDM -attending outpatient clinic Exclusion: -insulin-dependent DM -renal dysfunction -hepatic disorder -significant cardiac complications within 6 months -mental incompetence -history of non-compliance with regular clinic visits in past 2 years
Manage NIDDM diabetes in African-Americans Fasting plasma glucose and glycated hemoglobin concentrations
Pharmacist with full-prescribing authority for hypoglycemic agents
N=28 randomized -Diabetes-specific pharmacotherapeutic evaluation and dosage adjustment -Comprehensive and individualized patient education on diabetes and its complications -Training on the recognition and treatment of hypoglycemia and hyperglycemia -Medication counseling -Specific instructions on dietary regulation and an exercise plan -Training for self-monitoring of blood glucose -Adjusted or titrated hypoglycemic therapeutic regimens Mode/Frequency: -Follow-up on scheduled weekly basis until targeted glycemic control reached, then clinic visit every 2-4 weeks
N=17 randomized -reported to clinic for initial assessment and final exit visit -instructed to continue to receive standard care from PCP (every 3-4 months)
None reported
T2DM = type 2 diabetes; CAD = coronary artery disease; cRCT = cluster randomized controlled trial; CV = cardiovascular; LDL = low-density lipoprotein; VA = Veterans Affairs; KP = Kaiser Permanente; BP = blood pressure; DM = diabetes mellitus; SBP = systolic blood pressure; EMR = electronic medical record; SCHC = Siouxland Community Health Center; NIDDM = non-insulin-dependent diabetes mellitus; OTC = over the counter; PCP = primary care provider; HEDIS = healthcare effectiveness data and information set; HbA1c = glycosylated hemoglobin; ADA = American diabetes association; ED = emergency department; MTM = medication therapy management; DBP = diastolic blood pressure; RCT = randomized controlled trial
Pharmacist-led Chronic Disease Management Evidence-based Synthesis Program
109
Table 22. Drug-related Problems Outcomes – Diabetes Studies
Study Intervention (n) Control (n)
Inappropriate dosage/prescription
or omission % (n/N)
Ineffectiveness% (n/N)
Drug-drug or drug-disease interaction (describe) % (n/N)
Non-adherence to prescribed regimen % (n/N)
Clinical/adverse events % (n/N)
Pharmacy componen
t Control
Pharmacy componen
t Control
Pharmacy componen
t Control Pharmacy
component Control Pharmacy component Control
Skinner 2015 IG=2935 CG=29
NR NR NR NR NR NR Medication adherent (refilled at
least 85% of the time)
62%
7% (P<.001)
NR NR
Spence 201413 IG=359 CG=428
NR NR NR NR NR NR 53.5% (192/359) adherent
Mean MPR 0.78 (0.2)
Discontinued
11.7% (42/359)
37.4% (160/428) adherent (P=.001)
Mean MPR 0.74 (0.2) (P=.091)
Discontinued 35.5%
(152/428) (P=.001)
NR NR
Jacobs 201238 IG=72 CG=92
NR NR NR NR NR NR NR NR No adverse events caused by study protocol
Cohen 201132 IG=50 CG=49
NR NR NR NR NR NR Totala medication possession ratio: 0.87
0.83 (P=.19)
NR NR
Jameson 201036 IG=52 CG=51
NR NR NR NR NR NR NR NR 1 severe hypoglycemic event in intervention group (events could
not be assessed in control group)
Pharmacist-led Chronic Disease Management Evidence-based Synthesis Program
110
Study Intervention (n) Control (n)
Inappropriate dosage/prescription
or omission % (n/N)
Ineffectiveness% (n/N)
Drug-drug or drug-disease interaction (describe) % (n/N)
Non-adherence to prescribed regimen % (n/N)
Clinical/adverse events % (n/N)
Pharmacy componen
t Control
Pharmacy componen
t Control
Pharmacy componen
t Control Pharmacy
component Control Pharmacy component Control
Odegard 200551 IG=43 CG=34
Diabetes MedicationsMean (SD) MAI scores at baseline:
1.1 (1.5) 6 months: 0.6 (0.7) 1 year:
0.8 (1.0)
Mean MAI scores at baseline: 0.8 (1.0)
6 months: 0.8 (1.4) 1 year:
0.6 (0.7) Appropriate-
ness of diabetes
medications: P=.65
between groups over study period
NR NR NR NR Intervention had no effect on improving adherence during study
period
NR NR
Rothman 200539 IG=112, 6months 105, 1yr 99 CG=105, 6months 99, 1yr 95
NR NR NR NR NR NR NR NR Rate of events from 6-12
months follow-up
Hypoglycemic episodes 1.3 Hypotensive episodes 0.1
Hypoglycemic episodes 1.0
(Rate ratio 1.3 [0.6, 2.5])
Hypotensive episodes 0.2 (Rate ratio 0.3 ([0.1, 1.6])
Jaber 199637 IG=17 CG=22
NR NR NR NR NR NR NR NR 17 hypoglycemic reactions (mild to moderate; self-treated)
2 hypoglycemic reactions (mild to moderate; self-treated)
CG=control group; IG=intervention group; MAI=medication appropriateness index; NR = not reported a Antihypertensive, cholesterol, and diabetes medications
Pharmacist-led Chronic Disease Management Evidence-based Synthesis Program
111
Table 23. Mortality, Quality of Life, Access, and Patient Satisfaction Outcomes – Diabetes Studies
Study; Intervention (n) Control (n)
All-cause mortality % (n/N)
Health-related quality of life (describe) Access to care (describe) Patient satisfaction with care
(describe) Pharmacy
component Control Pharmacy component Control Pharmacy
component Control Pharmacy component Control
Cohen 201132 IG=50 CG=49
4% (2/50) 2% (1/49) P = NSb
VR-36 Mean
change: Physical
1.65 Mental 0.48 (both P=NS
from baseline)
Physical -1.95
Mental 0.78 (both P=NS
from baseline)
NR NR NR NR
Pape 201148 IG=3 clinics, 23 physicians, 2069 patients CG=6 clinics, 45 physicians, 4160 patients
NR NR NR NR Satisfaction with reaching
someone in an emergencya
84%
77% (P=.04)
Overall satisfaction a 5.4 (0.9)
5.2 (1.1) (P=.15)
Taveira 201130 IG=44 CG=44
All-cause NR No diabetes-related death in
either group
NR NR NR NR NR NR
Scott 200640 IG=64 CG=67
NR NR Total DQOL score -
change from baseline to
month 9 24.4
14.8 (P=NR)
NR NR DQOL score - satisfaction measure
- change from baseline to month 9
13.7
6.4 (P=.007)
Rothman 200539 IG=112, 6months 105, 1yr 99 CG=105, 6months 99, 1yr 95
1.8% (2/112)
3.8% (4/105) (P=.43)b
NR NR NR NR DTSQ +8 over 12 months
of intervention
+4 over 12 months of
intervention Difference: +3 (1, 6) (P<.05)
Jaber 199637 IG=17 CG=22
NR NR Groups similar for any domain of Health Status Questionnaire
(version 2.0)
NR NR NR NR
ADA = American Diabetes Association; CG = control group; DQOL=Diabetes Quality of life Questionnaire; DTSQ = Diabetes Treatment Satisfaction Questionnaire; IG = intervention group; NR = not reported; NS = not statistically significant; VR-36 = SF-36 for Veterans a Assessed using ADA and National Committee for Quality Assurance Provider Recognition Program Modified Patient Satisfaction Survey b Calculated P value (not reported in study)
Pharmacist-led Chronic Disease Management Evidence-based Synthesis Program
112
Table 24. Healthcare Utilization and Cost Outcomes – Diabetes Studies
Study; Intervention (n) Control (n)
Office visits Urgent care visits/
Emergency room (ER) visits
Hospitalizations Medications Costs or Other (describe)
Pharmacy componen
t Control
Pharmacy componen
t Control
Pharmacy componen
t Control Pharmacy
component Control Pharmacy
component Control McAdam-Marx 201553 IG=303 CG=394
Outpatient utilization: Mean (SD) difference pre to post intervention 1.16 (6.81)
0.61 (3.93) (P<.001) between groups
Mean (SD) difference pre to post intervention 0.07 (1.28)
0.04 (0.35) (P=.78) between groups
Inpatient utilization
Mean (SD) difference pre to post intervention -0.01 (0.69)
0.01 (0.30) (P=0.56) between groups
NR NR Total patient charges
Mean (SD) difference pre
to post intervention
$251 ($18,173)
$1,341 ($14,475) (P=0.04) between groups
Chung 201450 IG=220 CG=220
NR NR Increase of 4 visits per
220 patients from pre-index to
post-index year (mean
0.018)
Increase of 16 visits per
220 patients (mean 0.073) (P=.18)
Decrease of 1
hospital-ization for
220 patients from pre-index to
post-index year (mean
-0.005)
Increase of 8 hospital-izations for
220 patients (mean 0.036) (P=.06)
NR NR NR NR
Spence 201413 IG=359 CG=428
NR NR 1.7% (6/359)
14.2% (18/428) (P=.04)
0.6% (2/359)
1.4% (6/428) (P=.24)
NR NR $5.79 saved for every dollar spent on program
(including coronary artery disease program)
Brummel 201346 IG=121 CG=103
NR NR NR NR NR NR Daily Aspirin use
Baseline 97.5% Post
intervention 100%
Follow-up 99.2%
Baseline 93.3% Post
Intervention 98.1%
Follow-up 99.0%
(all P=NS between groups)
NR NR
Pharmacist-led Chronic Disease Management Evidence-based Synthesis Program
113
Study; Intervention (n) Control (n)
Office visits Urgent care visits/
Emergency room (ER) visits
Hospitalizations Medications Costs or Other (describe)
Pharmacy componen
t Control
Pharmacy componen
t Control
Pharmacy componen
t Control Pharmacy
component Control Pharmacy
component Control Ip 201343 IG=147 CG=147
NR NR NR NR NR NR NR NR 10 year CHD risk:
decreased from 16.4 to
9.3% 10 year
stroke risk: decreased from 7.6 to
6.8%
10 year CHD risk: decreased
from 17.4 to 14.8%
(P<.001 vs intervention) 10 year stroke risk: no change (P=.001 vs intervention)
Heisler 2010/201233,34 IG=1797 patients, 8 primary care teams CG=2303 patients, 8 primary care teams
Primary care visits mean (SD)
4.6 (5.9)
4.3 (6.1) (P=.10)
24% (434/1797)
23% (532/2303)
(P=.43)
13% (227/1797)
13% (300/2303)
(P=.71)
Proportion of patients with
BP medication changes 69.7%
(1253/1797)
Proportion of patients with
BP medication changes
63% (1451/2303)
(P<.01)
NR NR
Jacobs 201238 IG=72 CG=92
NR NR NR NR NR NR Increase in number of
meds during study period:
1.2
Number of meds at end of study: 7.1
Increase in number of
meds during study period: 0.9 (P=NS)
Number at end
of study: 6.0 (P=.03)
NR NR
Pharmacist-led Chronic Disease Management Evidence-based Synthesis Program
114
Study; Intervention (n) Control (n)
Office visits Urgent care visits/
Emergency room (ER) visits
Hospitalizations Medications Costs or Other (describe)
Pharmacy componen
t Control
Pharmacy componen
t Control
Pharmacy componen
t Control Pharmacy
component Control Pharmacy
component Control Salvo 201249 IG=69 CG=57
NR NR NR NR NR NR Increase in total daily
insulin dose: 33 units (mean) (P=.004
compared to control at end
of study)
Bolus insulin added for 11
patients
Bolus insulin added for 1
patient (P=NR)
Influenza vaccine 70%
(48/69)
Pneumo-coccal
vaccine 67% (46/69)
Dietitian visit 39% (27/69)
Influenza 52% (30/57)
(P=.03)
Pneumococcal 40% (23/57)
(P=.003)
Dietitian 16% (9/57) (P=.003)
Cohen 201132 IG=50 CG=49
PCP visits in 6 months
(mean) 1.56
1.65 (P=NR)
NR NR NR NR At 6 months: Total
antihyper-tensive meds 2.34 (1.22) Diabetes
meds 1.64 (0.78)
Cholesterol meds 1.00
(0.49)
At end: Total antihyper-
tensive meds 1.94 (1.18) (P<.001)
Diabetes meds 1.41 (0.73)
(P=.03) Cholesterol meds 0.86
(0.41) (P=.006)
NR NR
Padiyara 201145 IG=321 CG=321
NR NR NR NR NR NR Take an aspirin at
least 15x/month 280/321)
42.4% (136/321) (P<.001)
NR NR
Pape 201148 IG=3 clinics, 23 physicians, 2069 patients CG=6 clinics, 45 physicians, 4160 patients
NR NR NR NR NR NR Any lipid lowering
medication 77%
Statin prescription
75%
Any lipid lowering
medication 63% (P=.04)
Statin prescription 60% (P=.01)
NR NR
Pharmacist-led Chronic Disease Management Evidence-based Synthesis Program
115
Study; Intervention (n) Control (n)
Office visits Urgent care visits/
Emergency room (ER) visits
Hospitalizations Medications Costs or Other (describe)
Pharmacy componen
t Control
Pharmacy componen
t Control
Pharmacy componen
t Control Pharmacy
component Control Pharmacy
component Control Taveira 201130 IG=44 CG=44
0.3 (0.6) 0.3 (0.6) (P=.70)
All cause 39.5%
Diabetes-
related 2.3%
All cause 39.5% (P=NS)
Diabetes-
related 4.7%
(P=.60)
14% 16.3% (P=.80)
No admissions
were diabetes-related
Dose increase or initiation: antihyper-
tensive 68.2% antihyper-glycemic
agent 81.8% antihyper-lipidemic 52.3%
antidepres-sants 29.6%
Dose increase or initiation: antihyper-
tensive 34.9% (P=.003)
antihyper-glycemic agent
58.1% (P=.02)
antihyper-lipidemic
39.5% (P=.28) antidepres-sants 25.0%
(P=.81)
Over 6 months:
Mean of 6.6 medical
appointments Mean of 1.2 (0.8) PCP
visits
Mean of 1.3 (0.9) PCP
visits Mean of 0.6
(1.2) Diabetes
Self-Management Education
visits (P=NR)
Jameson 201036 IG=52 CG=51
NR NR NR NR NR NR Basal-bolus insulin started 28.8% (15/52) Discontinued
oral medication
28.8% (15/52)
Basal-bolus insulin started
2% (1/51) (P=.0002)a
Discontinued oral
medication 2% (1/51)
(P=.0002)a
NR NR
Taveira 201031 IG=58 CG=51
NR NR NR NR NR NR Aspirin added 5.3%
Statin added 7%
Insulin added 15.8%
Niacin added 17.5%
Aspirin added 4.0% (P=NS
between groups)
Statin added 5.9% (P<.05) Insulin added 2% (P<.05)
Niacin added 2% (P<.05)
NR NR
Pharmacist-led Chronic Disease Management Evidence-based Synthesis Program
116
Study; Intervention (n) Control (n)
Office visits Urgent care visits/
Emergency room (ER) visits
Hospitalizations Medications Costs or Other (describe)
Pharmacy componen
t Control
Pharmacy componen
t Control
Pharmacy componen
t Control Pharmacy
component Control Pharmacy
component Control Fox 200947 IG (MTM participants)=255 CG1 (MTM non-participants)=56 CG2 (Not MTM eligible, CDC)=1,803
NR NR NR NR NR NR Change in number of
prescriptions per month during year
post intervention
-4.08%
-2.84% (P=NR)
Change in year following intervention Total drug
costs -18.4%
Total Part D copay -4.0%
Total copay -5.5%
Total drug costs -7.0%
Total Part D copay 4.2%
Total copay -1.5%
(P=NR)
Scott 200640 IG=64 CG=67
NR NR Urgent Care: RR 0.8 (0.4, 1.6)
ER: RR 0.8 (0.5, 1.4)
NR NR Aspirin therapy
achieved: 81% (52/64)
46% (31/67) (P=.02)
NR NR
Odegard 200551 IG=43 CG=34
Mean (SD) 3.2 (1.5) over 12 months
5.4 (2.4) over 12 months (P=NR)
NR NR NR NR NR NR NR NR
Rothman 200539 IG=112, 6months 105, 1yr 99 CG=105, 6months 99, 1yr 95
Rate of event from 6-12 month follow-up
2.0
1.9 (Rate ratio 1.1 [0.9,
1.3])
Rate of event from 6-12 month follow-up,
Urgent care 0.2
ED visits 0.4
Urgent care 0.2 (Rate Ratio 0.8 [0.4, 1.6]) ED visits 0.5 (Rate Ratio 0.8 [0.5, 1.4])
Rate of event from 6-12 month follow-up
0.2
0.2 (Rate Ratio 1.1 [0.6, 2.0])
Use of aspirin at 12 months 91% (87/96)
Use of aspirin 58% (54/93) (P<.0001)
NR NR
Shane-McWhorter 200541 IG=176 CG=176
NR NR NR NR NR NR Aspirin prescribed
55.1% (97/176)
64.7% (114/176) (P=.08)a
Immuniza-tions
1.25/pt DM education documented
100% (176/176)
0.95/pt (P<.006)
19.3% (34/176) (P<.001)
Pharmacist-led Chronic Disease Management Evidence-based Synthesis Program
117
Study; Intervention (n) Control (n)
Office visits Urgent care visits/
Emergency room (ER) visits
Hospitalizations Medications Costs or Other (describe)
Pharmacy componen
t Control
Pharmacy componen
t Control
Pharmacy componen
t Control Pharmacy
component Control Pharmacy
component Control Stroup 200352 IG=30 CG=40
NR NR 6.7% (2/30) had 2 visits
over 2 years - both
diabetes related
27.5% (11/40) had
16 visits (P=.03)
8 patients had
diabetes- related visits
(P=.115)
14 admissions
in 13/30 patients (43%)
8 patients had
diabetes-related
admissions
32 admissions
in 20/40 patients (50%)
14 patients had
diabetes-related
admissions (P=.58 for
admissions; P=.29 for
DM related)
NR NR NR NR
Jaber 199637 IG=17 CG=22
NR NR NR NR 5.6% (1/17) hospitalizati
on (chest pain)
9.1% (2/22) hospitalizations (non-
DM related) (P=NS)a
38 pharma-cotherapeutic interventions (mean 2.2/pt)
9 pharma-cotherapeutic interventions (mean 0.4/pt)
(P=NR)
NR NR
BP = blood pressure; CG = control group; CHD = coronary heart disease; DM = diabetes mellitus; ED=emergency department; IG = intervention group; NR = not reported; PCP = primary care provider; SD = standard deviation a Calculated P value (not reported in study)
Pharmacist-led Chronic Disease Management Evidence-based Synthesis Program
118
Table 25. Goal Attainment Outcomes – Diabetes Studies
Study; Intervention (n) Control (n)
Patient Goal Attainment definition Percentage of patients attaining goal (n/N)
Pharmacy component Control Brummel 201346 IG=121 CG=103
HbA1c<7% LDL <100mg/dL
BP <130/80 mmHg Tobacco Free Optimal Score
HbA1c Baseline 43.8%b
Post intervention 73.55%a Follow-up 42.15%ab
LDL Baseline 63.64%
Post intervention 83.47%a Follow-up 79.34%
Blood Pressure Baseline 66.12%
Post intervention 71.07% Follow-up 76.03%
Tobacco Free Baseline 85.95% Post intervention 91.74%ab
Follow-up 91.74%b
Optimal Score Baseline 21.49%
Post Intervention 45.45% (P<.001) Follow-up 25.62% (P=.0002)
HbA1c Baseline 63.11%
Post Intervention 72.82% Follow-up 59.22%
LDL Baseline 65.05%
Post Intervention 73.79% Follow-up 73.79%
Blood Pressure Baseline 61.17%
Post Intervention 72.82% Follow-up 69.9%
Tobacco Free Baseline 79.61%
Post Intervention 81.55% Follow-up 82.52%
Optimal Score Baseline 24.27%
Post intervention 39.81% (P=.0002)
Follow-up 30.10% (P=.08) Ip 201343 IG=147 CG=147
HbA1c <7% LDL <100mg/dL
BP <130/80 mm Hg All three goals
At 12 months HbA1c 62.6% (OR 3.9, P<.0001)
LDL 85% (OR 2.0, P=.02) BP 61.9% (OR 2.0, P=.002)
All 3 36.7% (OR 3.2, P=.0004) P<.001 for each of the three, NSR for “all 3”
At 12 months HbA1c 28.6%
LDL 57.5% BP 43.5% All 3 9.5%
Jacobs 201238 IG=72 CG=92
HbA1c<7% LDL-C <100mg/dL BP<130/80 mm Hg
HbA1c 12 months 35% (19/55)
LDL-C 12 months 62% (32/52)
SBP 12 months 51% (29/57)
DBP 12 months 84% (48/57)
HbA1c 12 months 21% (14/67) (P=.11)
LDL-C 12 months 55% (24/44) (P=.54)
SBP 12 months 43% (30/70) (P=.38)
DBP 12 months 77% (54/70) (P=.37)
Salvo 201249 IG=69 CG=57
HbA1c <7% 20.3% 14% p=.48
Cohen 201132 IG=50 CG=49
Recommended by the ADA: SBP<130mm Hg LDL<100mg/dL
HbA1c<7%
HbA1c 40.8% (OR 2.73 [1.03, 7.26]) SBP 58% (OR 3.06 [1.31, 7.16])
LDL 82% Combined 16.0%
HbA1c 20.4% (P=.03) SBP 32.7% (P=.02) LDL 65.3% (P=.06)
Combined 4.1% (P=.049)
Pharmacist-led Chronic Disease Management Evidence-based Synthesis Program
119
Study; Intervention (n) Control (n)
Patient Goal Attainment definition Percentage of patients attaining goal (n/N)
Pharmacy component Control Padiyara 201145 IG=321 CG=321
BP<130/80 mm Hg LDL-C <100mg/dL
HbA1c <7% Documented A1c in last 6 months
Received formal diabetes education
44.6% (120/269) 76% (244/321)
50.8% (163/321) 100% (321/321) 93.4% (300/321)
48% (123/256) P=.43 59.2% (190/321) P<.001 71% (228/321) P<.001
99.7% (320/321) P=.317 40.2% (129/321) P<.001
Pape 201148 IG=3 clinics, 23 physicians, 2069 patients CG=6 clinics, 45 physicians, 4160 patients
LDL-C <100mg/dL HbA1c <7%
BP <130/80mm Hg
LDL-C 78% (OR 2.8 [2.2, 3.7]) HbA1c 51%
BP 55%
LDL-C 50% (P=.003) HbA1c 49% (P=.81)
BP 49% (P=.22)
Taveira 201130 IG=44 CG=44
ADA guidelines HbA1c<7%
SBP<130 mm Hg, DBP<80 mmHg Total cholesterol <200mg/dL HDL cholesterol<130mg/dL LDL cholesterol<100mg/dL
Change in proportion attaining goal: HbA1c 29.6% (P=.04) (OR 4.3 [1.2, 15.9])
SBP 31.8% LDL-C 18.2%
Non-HDL-C 27.9%
Change in proportion attaining goal: HbA1c 11.9%
SBP 14% (P=.10) LDL-C 13.6% (P=.53)
Non-HDL-C 22.7% (P=.39)
Jameson 201036 IG=52 CG=51
HbA1C decreased by at least 1% 67.3% (35/52) 41.2% (21/51) (P=.02)
Johnson 201042 IG=222 CG=262
HbA1c <7% HbA1c <8%
BP <130/80 mmHg LDL-C <100mg/dL
BMI 18.5-24.9 kg/m2
HbA1c <7% 43/222 (19.37%) (OR 4.04 [2.16, 7.56])
HbA1c< 8% 116/222 (52.25%) (OR 5.13 [2.22, 7.89])
BP <130/80 106/136 (77.94%) LDL-C 118/148 (79.73%)
BMI 41/115 (35.65%)
HbA1c <7% 17/162 (6.49%) P<.001 HbA1c <8% 52/262 (19.85%) P<.001 BP<130/80 156/251 (62.15%) P=.002
LDL-C<100 85/182 (46.7%)P<.001 BMI 113/248 (45.56%) P=.08
Taveira 201031 IG=58 CG=51
ADA guidelines HbA1c<7%
SBP<130 mm Hg, DBP<80 mmHg Non-HDL cholesterol<130mg/dL
LDL cholesterol<100mg/dL
HbA1c 40.4% SBP 65.5% DBP 87.9%
Non-HDL cholesterol 70.2% LDL cholesterol 77.2%
HbA1c 21.6% (P<.05) SBP 39.9% (P<.05) DBP 68.6% (P<.05)
Non-HDL cholesterol 62.8% (P=NS) LDL cholesterol 77.5% (P=NS)
Fox 200947 IG (MTM participants)=255 CG1 (MTM non-participants)=56 CG2 (Not MTM eligible, CDC)=1,803
LDL-C <100mg/dL 69% (176/255) CG1= 50% (28/56) CG2= 54.1% (976/1803) (P<.001)
Scott 200640 IG=64 CG=67
HbA1c <7% SBP <130 mmHg
HbA1c 67.2% (43/64) SBP 78% (50/64)
HbA1c 35.8% (24/67) (P=.05) SBP (numbers not reported) (P=.04)
Pharmacist-led Chronic Disease Management Evidence-based Synthesis Program
120
Study; Intervention (n) Control (n)
Patient Goal Attainment definition Percentage of patients attaining goal (n/N)
Pharmacy component Control Odegard 200551 IG=43 CG=34
American Diabetes Association target for diabetes control (HbA1c <7%)
8% 13% (P=.69)
Shane-McWhorter 200541 IG=176 CG=176
HbA1c <7% SBP <130 mmHg DBP <80 mm Hg
Total cholesterol <200mg/dL LDL<100 mg/dL TG <150mg/dL HDL >40mg/dL
HbA1c 58 (38.4%) SBP 66 (39.8%) DBP 65 (39.2%) TC 52 (61.9%) LDL 42 (53.2%) TG 28 (35.4%)
HDL 41 (51.9%)
HbA1c 48 (27.7%) P=.04 SBP 74 (42.1%) P=.67 DBP 80 (45.5%) P=.24 TC 45 (47.4%) P=.13 LDL 28 (42.4%) P=.20 TG 26 (28.5%) P=.42
HDL 59 (66.3%) P=.06 Kelly 200044 IG=32 CG=16
HgA1c HbA1c <7% SBP <130mmHg DBP <85mmHG
HbA1c 31.3% (10/32) SBP 43.8% (14/32) DBP 65.6% (21/32)
HbA1c 6.3% (1/16) (P=.03) SBP 12.5% (2/16) (P=.01)
DBP 62.5% (10/16) (P=.78) ADA = American Diabetes Association; BP = blood pressure; CG = control group; DBP = diastolic blood pressure; HbA1c = glycosylated hemoglobin; HDL(-C) = high-density lipoprotein (cholesterol); IG = intervention group; LDL(-C) = low-density lipoprotein (cholesterol); NR = not reported; SBP = systolic blood pressure; SMBG = self- monitored blood glucose; TC = total cholesterol; TG = triglycerides a significant change from year before b significantly different between groups
Pharmacist-led Chronic Disease Management Evidence-based Synthesis Program
121
Table 26. Study and Intervention Characteristics – Dyslipidemia Studies
Author, year Study design Type of Clinic
Target Population
Duration of
study/ follow-up
Inclusion/ Exclusion Criteria
Goal of Intervention
Primary
Outcome
Type of pharmacist Pharmacist Intervention Comparator
intervention Collaboration
Smith 201354 Retro Cohort Primary Care (VA)
Patients with uncontrolled LDL cholesterol based on NCEP/ ATPIII goal Maximum of 46 months (patients followed from index visit until LDL goal achieved or end of study period)
Inclusion: -patient seen in intervention or usual care (study) clinic -cholesterol-lowering medication changed or initiated during study period -random sample (~15%) chosen for study (225 in each group) Exclusion -index or final cholesterol values were missing
More effective and efficient lipid management compared to usual care Primary outcome: differences in mean final measured values of lipids and triglycerides between intervention and control cohorts
Clinical pharmacist, at least 1 year post-grad residency training
N=213 -Patients referred by clinician for further evaluation and adjustment of therapy -Pharmacists reviews results from laboratory tests and adjusted medications as necessary -Patient discharged from program when they reach individual NCEP/ATPIII goal Mode/Frequency: -patients seen by pharmacist for at least one visit -follow-up visits at 6- to 8-week intervals as needed
N=219 unmatched, groups randomly chosen from same population -Pharmacists provide drug information services and perform chart review for formulary management and cost-saving initiatives -Teaching clinic so patients followed more frequently (approx. 6- to 8-weeks) -No care management services
Physicians, nurse practitioners Pharmacists work with a group of practitioners to provide care management and drug information services
Miller 200855 Prospec-tive cohort Family medicine and other ambula-tory care (university-based)
Patients with dyslipidemia treated with atorvastatin 4 to 52 weeks (first fasting lipid panel after conversion to new statin regimen)
Inclusion: -enrolled in Colorado Indigent Care Program -diagnosis of dyslipidemia -treated with atorvastatin (prescribed by study clinic provider) Exclusion: -taking amiodarone, verapamil, cyclosporine, and/or gemfibrozil -history of transplantation or HIV -no fasting lipid panel before statin conversion -not adherent (based on refill history) with atorvastatin, or refused conversion
Improve outcomes following statin conversion Reduction in concentration of LDL and LDL goal attainment
Clinical pharmacy specialists and year-2 resident
N=30 Family medicine center patients: -Conducted individual medical review to identify goal -Reviewed patient LDL goal (NCEP ATP III); made therapeutic conversion to simvastatin, rosuvastatin, or ezetimibe-simvastatin (dose based on whether or not patient had achieved LDL goal on atorvastatin) Mode/Frequency: -Pharmacist did medication review, contacted patients to explain changes made -Patients asked to see PCP at 3 months (lipid panel, other tests)
N=87 unmatched Internal medicine, cardiology, and endocrinology clinic patients Usual care When refill request for atorvastatin received, pharmacy contacted provider to recommend equipotent conversion Recommendation was optional and final selection was made by provider
Pharmacist collaborated with prescribing physician to approve new regimen
Pharmacist-led Chronic Disease Management Evidence-based Synthesis Program
122
Author, year Study design Type of Clinic
Target Population
Duration of
study/ follow-up
Inclusion/ Exclusion Criteria
Goal of Intervention
Primary
Outcome
Type of pharmacist Pharmacist Intervention Comparator
intervention Collaboration
Mazzolini 200556 Retro cohort Outpatient clinics (VA)
Dyslipidemia Reviewed charts until reached goal of 115 patients in each group Followed at least 6 months after index visit
Inclusion: Intervention group -referred by primary care; referral is voluntary -randomly selected study patients from all attending lipid education class Control group -randomly selected from patients seen in primary care with diagnosis of dyslipidemia Both groups -diagnosis of dyslipidemia -≥3 visits with pharmacist or primary care -followed ≥6 months -enrolled in VA ≥1 year Exclusion: -documented non-compliance with appointments -TSH > 4.5 m IU/ml any time during study period
Compare outcomes with pharmacist-managed clinic vs care by other health professionals Primary: Absolute values and percentage changes in LDL; proportion attaining LDL goal
Clinical pharmacists with prescribing authority for all VA formulary lipid-lowering agents; perform all changes to lipid-lowering medications once patient enrolls in lipid clinic
N=115 -Assessed and treated dyslipidemia to achieve goals based on NCEP ATP III guidelines and recent recommendations -Education including treatment of dyslipidemia and therapeutic lifestyle modifications -Follow-up visits: discuss patient’s lifestyle; changes in health status and current lipid profile reviewed; medication changes made if needed -Discharged if goal lipid levels maintained for 2 or more consecutive clinic visits Mode/Frequency: -Initial visit at clinic including class session -Scheduled for follow-up visits in the clinic
N=115 unmatched, randomly selected Usual care
Physicians, physician assistants, nurse practitioners Dietitians (education sessions)
Pharmacist-led Chronic Disease Management Evidence-based Synthesis Program
123
Author, year Study design Type of Clinic
Target Population
Duration of
study/ follow-up
Inclusion/ Exclusion Criteria
Goal of Intervention
Primary
Outcome
Type of pharmacist Pharmacist Intervention Comparator
intervention Collaboration
Straka 200557 CCT Staff-model HMO clinics
Coronary heart disease (CHD) At least 6 months follow-up after enrollment Post-study follow-up of 18 months to assess sustainability
Inclusion: -age ≥18 -CHD and LDL levels not at goal (<100 mg/dL) Intervention group included 1st 166 patients (of 359 eligible) who signed consent form (16 subsequently excluded) Control group included all eligible patients
Manage hyper-cholesterolemia in patients with CHD Primary: changes in magnitude of LDL, percentage achieving goal LDL levels
Clinical pharmacists
N=150 -Pharmacist and primary care provider cooperatively developed patient-specific care plan (implemented if physician approved and patient consented) -Pharmacist implemented plan:
-prescribing and adjusting dosages -obtaining fasting lipid panel -evaluating and setting up all lipid panels -working through dosage titrations -communicating actions, recommendations, findings to physician -educating patients about risk/benefits of new or adjusted dosages -providing advice about aspirin, diet, weight loss, exercise -referring to other resources (smoking cessation, dietary counseling)
Mode/Frequency: -Pharmacist met with PCP to come up with plan -Patients contacted by telephone to follow-up for tests, to notify them of changes, and for education -Lipid panel/liver tests at baseline and then every 6 weeks, after stabilizing liver tests every 3-6 months, fasting lipid panel annually
N=331 Usual care (no clinical pharmacist providing oversight)
-Pharmacist and primary care provider cooperatively developed patient-specific care plan (implemented if physician approved and patient consented) -Communicated actions, recommenda-tions, findings to physician
Pharmacist-led Chronic Disease Management Evidence-based Synthesis Program
124
Author, year Study design Type of Clinic
Target Population
Duration of
study/ follow-up
Inclusion/ Exclusion Criteria
Goal of Intervention
Primary
Outcome
Type of pharmacist Pharmacist Intervention Comparator
intervention Collaboration
Ellis 200058 RCT – IMPROVE substudy Primary care at 9 VA Medical Centers
Dyslipidemia 12 months
IMPROVE Inclusion: -high risk for drug-related adverse events (meeting 3+ of following a. ≥5 drugs in regimen, b. ≥12 doses/day, c. ≥4 drug changes in past year, d. ≥3 concurrent diseases, e. history of noncompliance, f. treatment with drugs requiring monitoring) -VAMC patient ≥12 months -expected to continue VAMC care -residence close to VAMC -working telephone SUB-STUDY: -diagnosis of dyslipidemia Exclusion: -seen in pharmacist-managed clinics in past 12 months -life expectancy <12 months -psychiatric diagnosis requiring services of mental health clinic -poor English -visually impaired
LDL < 100 mg/dl for secondary prevention in patients with coronary artery disease or diabetes LDL < 130 mg/dl for all others Primary outcome not specified
Ambulatory care clinical pharmacists
N=208 with dyslipidemia Pharmaceutical care in addition to usual medical care -Drug assessments -Adjustments to medications to improve care and disease control -Identify and prevent drug-related problems -Exact role varied depending on scope of practice (eg, adjust drug therapy, order lab tests) (NOTE: pharmacist intervention not limited to dyslipidemia) Mode/Frequency: -Initial visit -Follow-up at least 3 times for at least 12 months -Intervention continued until goals were met (patient-specific goals developed with physician and pharmacist)
N=229 with dyslipidemia Usual care
Patient goals developed with physician
Pharmacist-led Chronic Disease Management Evidence-based Synthesis Program
125
Author, year Study design Type of Clinic
Target Population
Duration of
study/ follow-up
Inclusion/ Exclusion Criteria
Goal of Intervention
Primary
Outcome
Type of pharmacist Pharmacist Intervention Comparator
intervention Collaboration
Bogden 199759 RCT University-affiliated primary care teaching clinic
High total cholesterol 6 months
Inclusion: -total cholesterol ≥ 240 mg/dL within 6 months before randomization Exclusion: -minors -patients unable to sign consent form
Lower cholesterol levels and meet NCEP goals (pharmacist and physician teamwork) Change in total cholesterol from baseline level
NR N=50 -Recommendations to physicians on dosage, drug selection (eg, least costly regimen), monitoring -Meeting prior to PCP visit
-medication history -answer questions -encourage compliance -review laboratory data
Mode/Frequency: -30-minute meeting with patients before their physician visit -Clinic visits at 0 and 6 months, interim visits also occurred
N=50 Usual care (including access to pharmacy clerk at patient request)
Pharmacist gave recommenda-tions to physician
Konzem 199760 CCT Primary care (VA)
Patients with hypercholesterolemia 52 weeks
Inclusion: -Diagnosis of hyper-cholesterolemia -prescribed colestipol hydrochloride oral suspension -not presently receiving any other lipid-lowering drugs -fasting lipid profile within 1 month before starting colestipol
Enhance patient acceptance and compliance with therapy and improve outcomes Primary outcome not specified
Pharmacists who had received training on intervention tasks
N=17 (3 lost to follow-up) -Therapy managed by pharmacist and physician (referred by physician) -Pharmacist provided
-education -titrated dosages -dietary analysis
-Telephone contacts to encourage compliance and evaluate acceptance of regimen -Data collection at 26, 52 weeks Mode/Frequency: -Initial visit -Contacted patients by telephone 2, 4, and 6 weeks after initial visit -Follow-up visit at 8 weeks to evaluate lab results and acceptance
N=20 Usual care, provided by physician; received drug counseling (what agent is for, instructions for taking) but no other contact from pharmacist
Physicians
ACE = angiotensin converting enzyme; BP = blood pressure; CAD = coronary artery disease; CHF = congestive heart failure; COPD = chronic obstructive pulmonary disease; CPCRS = Clinical Pharmacy Cardiac Risk Service; DRP = drug related problem; ED = emergency department; EF = ejection fraction; EMR = electronic medical record; ESRD = end stage renal disease; HbA1c = glycosylated hemoglobin; HF = heart failure; HTN = hypertension; LDL-C = low-density lipoprotein cholesterol; HDL-C = high-density lipoprotein cholesterol; QOL = quality of life; TSH = thyroid-stimulating hormone
Pharmacist-led Chronic Disease Management Evidence-based Synthesis Program
126
Table 27. Drug-related Problems Outcomes – Dyslipidemia Studies
Study Intervention (n) Control (n)
Inappropriate dosage/prescription or omission
% (n/N) Ineffectiveness% (n/N) Drug-drug or drug-disease
interaction (describe) % (n/N) Non-adherence to
prescribed regimen (n/N) Clinical/adverse events % (n/N)
Pharmacy componen
t Control
Pharmacy componen
t Control
Pharmacy componen
t Control
Pharmacy componen
t Control
Pharmacy componen
t Control
Konzem 199760 IG=17 CG=20
NR NR NR NR NR NR Compliance 89% (9.2%)
n=14
NR NR NR
CG = control group; IG = intervention group
Table 28. Mortality, Quality of Life, Access, and Patient Satisfaction Outcomes – Dyslipidemia Studies
Study; Intervention (n) Control (n)
All-cause mortality% (n/N) Health-related quality of life (describe) Access to care (describe) Patient satisfaction with care
(describe) Pharmacy
component Control Pharmacy component Control Pharmacy
component Control Pharmacy component Control
No studies reported CG = control group; IG = intervention group
Table 29. Healthcare Utilization and Cost Outcomes – Dyslipidemia Studies
Study; Intervention (n) Control (n)
Office visits Urgent care visits/
Emergency room (ER) visits
Hospitalizations Medications Costs or Other (describe)
Pharmacy componen
t Control
Pharmacy componen
t Control
Pharmacy componen
t Control Pharmacy
component Control Pharmacy
component Control Smith 2013 IG=21354 CG=219
Mean number of visits per patient
2.0 (1.3)
2.0 (1.3) P = .77
NR NR NR NR Mean number of
interventions per patient
(eg, medication changes) 1.1 (1.8)
0.7 (1.1) (P=.002)
NR NR
Pharmacist-led Chronic Disease Management Evidence-based Synthesis Program
127
Study; Intervention (n) Control (n)
Office visits Urgent care visits/
Emergency room (ER) visits
Hospitalizations Medications Costs or Other (describe)
Pharmacy componen
t Control
Pharmacy componen
t Control
Pharmacy componen
t Control Pharmacy
component Control Pharmacy
component Control Miller 200855 IG=30 CG=87
NR NR NR NR NR NR Post-conversion change in potency
Higher: 23% Equivalent:
70% Lower 7%
Higher: 16% Equivalent:
48% Lower: 36%
NR NR
Mazzolini 200556 IG=115 CG=115
Annual visits 2.97
2.98 (P=.06)
NR NR NR NR Use of lipid-lowering
agent 94%
(108/115)
24% (28/115)
(P<.0001)a
NR NR
Straka 200557 IG=150 CG=331
NR NR NR NR NR NR Use of lipid lowering therapy
Pre-intervention:
57% (86/150)
Post: 78%
(117/150)
Pre-intervention:
48% (158/331) Post: 44% (146/331) (P<.0001 between
groups post-intervention)
NR NR
Ellis 200058 IG=208 CG=229
Physician visits
Baseline 769
12 months 799
Physician visits
Baseline 850
12 months 925
NR NR NR NR NR NR Mean changes in costs from year before to
year after randomization Total: $1583
Hospitalizations: $710
Clinic visits: $302
All drugs: $269
Total: $1213 Hospitaliza-tions: $670 Clinic visits:
$372 All drugs:
$106
All differences in
change in mean
(P>.05)
Pharmacist-led Chronic Disease Management Evidence-based Synthesis Program
128
Study; Intervention (n) Control (n)
Office visits Urgent care visits/
Emergency room (ER) visits
Hospitalizations Medications Costs or Other (describe)
Pharmacy componen
t Control
Pharmacy componen
t Control
Pharmacy componen
t Control Pharmacy
component Control Pharmacy
component Control Bogden 199759 IG=50 CG=50
Mean of 12 clinic visits
Mean of 9 visits
(P<.05)
Reported frequencies of ER visits did not differ significantly between
groups
NR NR 27 medications
started 21
medications discontinued
16 dose increases
NR Mean medication
charge in last month $11.40
decrease per patient from 1st
month
$3.82 increase (P=NS)
Konzem 199760 IG=17 CG=20
NR NR NR NR NR NR Percent continuing colestipol 8 weeks:
80% 52 weeks:
65% Mean (std)
dosage (g/day) at 8
weeks: 18 (4)
52 weeks: 13 (5)
Continuing 8 weeks:
70% 52 weeks:
40% (P<.05 at 52
weeks) Dosage 8 weeks:
10 (3) 52 weeks:
9 (2) (both P<.05)
NOTE: discontinued because of side effects, noncompli-ance, and
dissatisfac-tion
NR NR
CG = control group; IG = intervention group a Calculated P value (not reported in study)
Pharmacist-led Chronic Disease Management Evidence-based Synthesis Program
129
Table 30. Goal Attainment Outcomes – Dyslipidemia Studies
Study; Intervention (n) Control (n)
Patient Goal Attainment definition Percentage of patients attaining goal (n/N)
Pharmacy component Control Smith 201354 IG=213 CG=219
Individually set LDL goals based on NCEP/ATP III guidelines
80.3% OR 2.6 (95% CI 1.6, 4.3), P<.001
65.3%
Miller 200855 IG=30 CG=87
LDL goal based on risk factors Pre-conversion: 80% Post: 97%
(P=.04, pre vs post)
Pre-conversion: 90% Post: 75%
(P=.01, pre vs post) Mazzolini 200556 IG=115 CG=115
LDL goal TC
HDL TG
64.3% Change: 45.2% to 82.6% P<.001
43.5% to 23.5% P=.002 56.5% to 65.2% P=.224
15.7% (P<.001)
Straka 200557 IG=150 CG=331
LDL < 100 mg/dl 72% Difference remained significant after 18 months
post-intervention follow-up
18% (P<.001)
Ellis 200058 IG=208 CG=229
LDL < 100 mg/dl Baseline: 26% (23/89) Follow-up: 40% (49/124)
Baseline: 22% (24/107) Follow-up: 35% (40/116)
P=.97 for difference between groups at end of study
Bogden 199759 IG=50 CG=50
LDL goals based on comorbid conditions and risk factors (< 160 mg/dL, < 130 mg/dL, or < 100 mg/dL)
Total Group: 43% (20/27)
Goal of <160 or <130 mg/dL 38% (13/34)
Goal of < 100 mg/dL 54% (7/13)
21% (10/47) (P<.05)
14% (5/36) (P<.05)
45% (5/11) (P>.05)
Konzem 199760 IG=17 CG=20
LDL goal at week 8
LDL goal at week 52
42%
29%
15%
5% (P<.05) CG = control group; IG = intervention group; LDL = low-density lipoprotein; OR = odds ratio
Pharmacist-led Chronic Disease Management Evidence-based Synthesis Program
130
Table 31. Study and Intervention Characteristics – Hypertension Studies
Author, year Study design Type of Clinic
Target Population
Duration of Study/
Follow-up
Inclusion/Exclusion Criteria
Goal of Intervention
Primary Outcome
Type of Pharmacist Pharmacist Intervention Comparator
Intervention Collaboration
Carter 201561 CAPTION
cRCT
32 primary care offices
Uncontrolled hypertension (focus on minorities)
Randomized by office, office must have had an onsite clinical pharmacist
Inclusion: -English or Spanish speaking -age >18 years -uncontrolled BP (>140/90mmHg or >130/80 mmHg for patients with DM or CKD) Exclusion: -current signs of hypertensive emergency (acute angina, stroke, or renal failure) -systolic >200mmHg or diastolic >114mmHg -history of MI, stroke, or angina (past 6 months) -systolic dysfunction (LVEF <35%) -GFR <20mL/min -cirrhosis -hepatitis B or C infection or laboratory abnormality in past 6 months -pregnancy -pulmonary hypertension or sleep apnea (unless treated) -life expectancy < 2 years -residence in nursing home or dementia -inability to give consent or impaired cognitive function
BP control
Blood pressure control at 9 months
Clinical pharmacist
N=194 Brief intervention (9 months) N=207 Sustained intervention (24 months) Interventions were the same -Medical record reviewed by pharmacist -Structured interview -Medication history -Assessment of knowledge of BP medications, dosages, timing, potential side effects, barriers to adherence -Create care plan with recommendations for physician to adjust therapy and recommendations for patients for medication education, improving adherence, and strategies for lifestyle modification
Mode/Frequency: -Phone call at 2 weeks -Structured face-to-face visits at baseline, 1,2, 4, 6, and 8 months with options for additional visits
N=224 Usual care: Pharmacists instructed to avoid intervention for study participants but could provide usual care curbside consultations if physicians specifically asked; control offices participated in an alternative distracter intervention for asthma
-Pharmacist created care plan; shared with physician who could accept, reject, or modify
Pharmacist-led Chronic Disease Management Evidence-based Synthesis Program
131
Author, year Study design Type of Clinic
Target Population
Duration of
Study/ Follow-up
Inclusion/Exclusion Criteria
Goal of Intervention
Primary
Outcome
Type of Pharmacist Pharmacist Intervention Comparator
Intervention Collaboration
Zillich 201566 Retro-spective case-control Urban Midwest VA Medical Center, primary care clinics with PACT teamlets
HTN, referred to care manage-ment program 12 months
Cases: patients with HTN referred to care management program Controls: patients with HTN not referred to program
Evaluate pharmacists HTN care management program with PCMH Differences in systolic and diastolic BP levels at 6 and 12 months follow-up
Clinical pharmacists
N=465 Scope of practice allowed pharmacists to: -meet individually with patients -provide patient education -initiate, change, and discontinue medications Mode/Frequency: -Initial face-to-face visit with pharmacist -Patient discharged from program when BP goals attained -No information provided on mode or frequency of contacts after initial visit
N=1268 (Matched [maximum of 3:1] on physician, age, gender, diagnosis of DM and CKD, baseline systolic BP, number of HTN medications)Usual care
PCP referred patients to pharmacist
Hirsch 201469 RCT (pragmatic) University-based primary care clinic
Uncontrolled HTN 6 and 9 months
Inclusion: -age ≥18 years -diagnosis of HTN with most recent BP measurement ≥140/≥90 mm Hg (≥130/≥80 mm Hg for DM) -current treatment with ≥1 anti-HTN medication -continuous active status with the clinic (defined as having a record of at least 1 visit in the 6 months before screening) Exclusion: -did not meet provisions of the clinical collaborative-practice protocol
BP control Mean change in BP from baseline
Clinical with >1y of pharmacy practice residency training and >7y experience in ambulatory care
N=75 Medication-therapy management (MTM) -Pharmacist could initiate, change, or discontinue medication therapy for management of uncontrolled HTN -Assessed patient knowledge of HTN and current treatment -Reviewed treatment goals, self-monitoring behavior, medical and medication history -Helped patient set goals. -Follow-up - reviewed progress toward goals, lab values, and adherence Therapeutic decisions and timing of patients’ laboratory testing and follow-up visits left to pharmacists’ clinical opinion, in consultation with physician if needed Mode/Frequency: -4 30-minute pharmacist visits (baseline, 3, 6, & 9 months), independent of PCP visits, and other contacts (clinic or telephone) as needed for follow-up with pharmacist
N=91 Usual care
Internal medicine physician -visits documented in EMR and shared
Pharmacist-led Chronic Disease Management Evidence-based Synthesis Program
132
Author, year Study design Type of Clinic
Target Population
Duration of
Study/ Follow-up
Inclusion/Exclusion Criteria
Goal of Intervention
Primary
Outcome
Type of Pharmacist Pharmacist Intervention Comparator
Intervention Collaboration
Magid 201370 RCT (pragmatic) HMO based primary care clinic
HTN with higher than recommended BP 6 months
Inclusion: -age 18 to 79 years -diagnosis of HTN - 2 most recent BP readings ≥140/≥90 mm Hg (≥130/≥80 mm Hg for DM or CKD) -prescribed ≤3 anti-HTN medications -had computer/internet access. Exclusion: -limited life expectancy -recent MI, stroke, percutaneous coronary intervention, or coronary artery bypass graft surgery -ESRD -not English speaking
BP control Proportion of patients who attained their goal BP at the 6-month clinic visit
Clinical N=175 American Heart Association Heart360 Web-enabled home BP monitoring intervention -Educational materials -Pharmacist met with patient and reviewed medication regimen, home BP measurements and adherence to anti-HTN medications -Made medication adjustments/changes as needed -Counseled on lifestyle changes Mode/Frequency: -Baseline and 6 months visits plus weekly review of BP summary reports
N=173 Usual care PCP follow-up and educational materials
Primary care physician, medication changes communicated via EMR
Margolis 201362 RCT (cluster) HMO based primary care clinic
Uncontrolled HTN 12 months Plus 6 months post-intervention follow-up
Inclusion: -uncontrolled HTN (≥140/≥90 mm Hg or ≥130/≥80 mm Hg for DM or CKD) at 2 most recent primary care visits in previous year Exclusion: -stage 4/5 kidney disease or ratio of albumin to creatinine of ≥700 mg/g -acute coronary syndrome, coronary revascularization, or stroke ≤3 months -known secondary causes of HTN -NYHA class III or IV CHF -known left ventricular ejection fraction <30% -pregnant
BP control Proportion of patients who attained their goal BP
Trained clinical
N=228, 8 clinics Intervention patients received home BP telemonitors -Transmitted BP data to pharmacists; anti-hypertensive therapy adjusted accordingly -1 hour in-person visit: reviewed history, education -Patient given individualized home BP goal -Telephone visits (every 2-4 wks)
-pharmacists emphasized lifestyle changes and medication adherence -assessed and adjusted anti-hypertension therapy (with algorithms) -managed adverse effects
Mode/Frequency: -First 6 months: met every 2 weeks via telephone until BP control sustained for 6 weeks; then monthly visits -During intervention months 7 through 12, telephone visits occurred every 2 months
N=222, 8 clinics Usual care
Primary care physicians
Pharmacist-led Chronic Disease Management Evidence-based Synthesis Program
133
Author, year Study design Type of Clinic
Target Population
Duration of
Study/ Follow-up
Inclusion/Exclusion Criteria
Goal of Intervention
Primary
Outcome
Type of Pharmacist Pharmacist Intervention Comparator
Intervention Collaboration
Magid 201167 RCT VA, City/ county, and HMO based primary care clinics
HTN 6 months
Inclusion: - HTN -taking ≤4 anti-HTN meds -elevations in 2 of 3 most recent electronic BP measurements (>140/>90 mm Hg; for patients with DM/CKD, >130/80 mm Hg)
BP control Proportion of patients who attained their goal BP and mean change in BP from baseline
Clinical N=174 Clinical pharmacist management of HTN with physician oversight -Patient education -Counseling on healthy therapeutic lifestyle changes -Pharmacist practiced under pre-approved drug therapy management protocols -Pharmacists reviewed home BP measurements, adherence to meds -Made medication adjustments as needed Mode/Frequency: -Baseline and 6 months visits plus weekly review of BP summary reports; if essential HTN, average home readings >135/85 mm Hg triggered pharmacist intervention (>125/75 mm Hg if diabetes or CKD)
N=164 Usual care
Primary care physician, notified of changes via EMR/phone
Carter 200963 RCT (prospective cluster) Community-based family medicine residency program clinics
HTN 6 months
Inclusion: -age ≥21 years -essential HTN -taking 0-3 anti-HTN meds -if no DM: clinic systolic BP 140-179 mm Hg or clinic diastolic BP 90-109 mm Hg (130-179 mm Hg or 80-109 mm Hg with DM) Exclusion: -BP medication or dose change ≤4 weeks prior to base-line visit -BP >180/110 mm Hg -evidence of hypertensive urgency or emergency -recent MI or stroke (within 6 months before enrollment) -NYHA class III/IV CHF, unstable angina, renal/hepatic disease -life expectancy <3 years -dementia/cognitive impairment
BP control Change in guideline adherence scores, % of patients with controlled BP, difference in mean systolic and diastolic BPs
Clinical -Residency in primary care
N=192, 3 clinics Pharmacists were encouraged to: -Assess medications and BP at baseline and at 1 month, at 3 months, and more frequently if necessary -Pharmacists made recommendations consistent with national guidelines Mode/Frequency: -Baseline, 3, and 6 months -Pharmacists were encouraged to assess medications and BP more frequently if necessary
N=210, 3 clinics Usual care (Passive observation group (intervention sites only) n=191)
Physicians (and research nurses) -Collaboration on how to best implement intervention -Pharmacists almost always provided face-to-face recommenda-tions to PCP -Physician education if necessary -All therapy changes approved by physician
Pharmacist-led Chronic Disease Management Evidence-based Synthesis Program
134
Author, year Study design Type of Clinic
Target Population
Duration of
Study/ Follow-up
Inclusion/Exclusion Criteria
Goal of Intervention
Primary
Outcome
Type of Pharmacist Pharmacist Intervention Comparator
Intervention Collaboration
Carter 200864 RCT prospective (cluster) University-based primary care clinics
HTN 9 months
Inclusion: -age 21-85 years -HTN: if no DM clinic BP 145-179 mm Hg/ 95-109 mm Hg (135-179 mm Hg or 85-109 mm Hg for patients with DM) Exclusion: -BP medication or dose change ≤4 weeks prior to baseline visit -enrollment in 24-hour BP monitoring consult service ≤ 6 months -stage 3 HTN (BP >180/110 mm Hg) -evidence of hypertensive urgency or emergency -recent MI or stroke (within 6 months before enrollment) -NYHA class III or IV CHF, unstable angina, serious renal or hepatic disease -poor prognosis (life expect. <3 years) -dementia or cognitive impairment
BP control Difference in mean systolic and diastolic BPs and proportion of patients with controlled BP
Clinical N=101, 2 clinics Patient interview at baseline by clinical pharmacist -Assessed patient’s regimen, suggested goal BP value, and provided recommendations to improve BP control -Primary focus of pharmacist was to address suboptimal medication regimens -Recommended adherence aids -Educated patients and/or taught them home monitoring -Made patient-specific recommendations -Recommend therapies consistent with JNC 7 guidelines Mode/Frequency: -Pharmacists encouraged to attend each clinic visit (2, 4, 6, and 8 months) and encouraged to initiate additional visits or telephone contact if BP remained uncontrolled
N=78, 3 clinics Usual care
Physicians (and nurses) -Pharmacist educated physician and made recommenda-tions -Pharmacists could not independently prescribe therapy; all changes approved by physician -Most recommenda-tions to physician performed face-to-face during patient visit; some physicians provided authority for pharmacists to make dosage changes and inform PCP immediately after visit
Pharmacist-led Chronic Disease Management Evidence-based Synthesis Program
135
Author, year Study design Type of Clinic
Target Population
Duration of
Study/ Follow-up
Inclusion/Exclusion Criteria
Goal of Intervention
Primary
Outcome
Type of Pharmacist Pharmacist Intervention Comparator
Intervention Collaboration
Green 200871 Ralston 201474* RCT Nonprofit, HMO-based primary care clinics *Sub-study with n=186 (intervention group), n=197 (control group – all home BP and Web)
HTN 12 months
Inclusion: -age 25-75 years -HTN diagnosis -taking antihypertensive meds -no diagnoses of DM, CVD or renal disease, or other serious conditions Eligible and willing patients were invited to 2 screening visits at their clinic. If mean diastolic BP (last 2 of 3 BP recordings, with the first measurement dropped) was between 90-109 mm Hg or mean systolic BP was between 140-199 mm Hg at both screening visits, participant was eligible for the study
BP control Difference in mean systolic and diastolic BPs and proportion of patients with controlled BP
Clinical N=261 Pharmacist care plus home BP monitoring, and web training -1 planned telephone visit to obtain a more detailed medication history and review allergies, intolerances, and CV risk factors -Introduced patient to action plan, a template with 5 components: 1) instructions for home BP monitoring 2) list of current medications 3) ≥1 patient-selected lifestyle goal(s) from the list in the Group Health HTN pamphlet 4) recommended medication changes based on stepped medication protocols 5) follow-up plan -Planned communication occurred over web every 2 weeks until BP controlled -Responded to patients with specific recommendations (including medication changes) Mode/Frequency: -Baseline and 12 months -All planned communications occurred over web every 2 weeks until BP controlled and less often thereafter
1) N=258 Usual care 2) N=259 Home BP monitoring and web training only
Pharmacist communicated with physician, all clinical concerns or potential deviations from the medication protocol were referred back to PCP
Pharmacist-led Chronic Disease Management Evidence-based Synthesis Program
136
Author, year Study design Type of Clinic
Target Population
Duration of
Study/ Follow-up
Inclusion/Exclusion Criteria
Goal of Intervention
Primary
Outcome
Type of Pharmacist Pharmacist Intervention Comparator
Intervention Collaboration
Hunt 200872 RCT Nonprofit integrated system, primary care clinics
HTN and uncontrolled blood pressure 12 months
Inclusion: -HTN and uncontrolled BP, -office visit within past 2 years (problem list entry of hypertension (ICD-9 of 410.*) -last systolic BP ≥160 mm Hg and/or a last diastolic BP ≥100 mm Hg) Exclusion: -no BP reading in chart in previous 2 years -attended a visit with a pharmacy practitioner in previous 6 months
BP control Difference in mean systolic and diastolic BPs
Clinical N=230 Pharmacists: -Reviewed subjects’ medications and lifestyle habits -Assessed vital signs -Screened for adverse drug reactions -Identified barriers to adherence -Provided education -Optimized anti-HTN regimen (titrating dose of existing medication, adding new agent, switching medication, or consolidating anti-HTN therapy) -Follow-up appointments as needed -Accessed patients’ medical records to assist medication selection and dosing Mode/Frequency: -Baseline visit with pharmacist -Follow-up appointments as necessary
N=233 Usual care
Physician available to discuss HTN treatment plan/other medical issues as needed; notes from visit communicated via EMR
Borenstein 200373 RCT Community hospital
HTN uncontrolled 12 months
Inclusion: -age ≥18 years -capitated medical insurance -diagnosis code for HTN -uncontrolled HTN (>140/90 of <65 years old or >160/90 if >65 years old) based on last recorded measure(s) Exclusion: -advanced dementia, terminal illness, organ transplantation, or secondary hypertension -absence of recorded blood pressure measurements
BP control Difference in mean systolic and diastolic BPs
Clinical N=98 -Pharmacists:
-Determined BP -Collected patient assessments for adherence, potential drug side effects, and relevant patient habits (tobacco use, diet, and exercise), per JNC V guidelines
-During clinic, pharmacists reviewed drug side effects and provided education regarding individualized dietary and lifestyle modifications -Called patient’s physician/covering physician, with findings and made treatment recommendations in accordance with evidence-based treatment algorithm Mode/Frequency: -Follow-up visits every 2-4 weeks at discretion of pharmacist (as often as necessary until BP control achieved)
N=99 Usual care
Physician; physicians made all final treatment decisions
Pharmacist-led Chronic Disease Management Evidence-based Synthesis Program
137
Author, year Study design Type of Clinic
Target Population
Duration of
Study/ Follow-up
Inclusion/Exclusion Criteria
Goal of Intervention
Primary
Outcome
Type of Pharmacist Pharmacist Intervention Comparator
Intervention Collaboration
Vivian 200268 RCT Veterans Affairs Medical Center
HTN 6 months
Inclusion: -stage 1, 2, or 3 hypertension as defined by JNC VI (>140 systolic or >90 diastolic) -age ≥18 -receiving anti-hypertension drug therapy -not receiving care at pharmacist-managed clinic Exclusion: -secondary cause of hypertension (CKD, renovascular disease, pheochromocytoma, Cushing’s syndrome, and primary aldosteronism) -missed >3 appointments in last year -were in hypertensive crisis (systolic BP >210 mm Hg or diastolic BP >110 mm Hg) -NYHA class III or IV CHF, ESRD, psychiatric disorder, severe hepatic dysfunction, terminal cancer, or other condition with life expectancy to <1 year
BP control Difference in mean systolic and diastolic BPs and proportion of patients with controlled BP
Clinical N=27 Pharmacist -Prescribing authority -Made appropriate drug therapy changes (in both drug selection and dosage) for blood pressure control in accordance with JNC VI -Did not make any changes in patients’ other drugs that may adversely affect blood pressure (eg, venlafaxine, sibutramine) -Drug counseling provided at each visit (thorough discussion about side effects, recommended lifestyle changes, an assessment of compliance) Mode/Frequency: -Saw pharmacist 1 time/month
N=29 Usual care -Traditional pharmacist services (eg, distribution)
Not reported
Pharmacist-led Chronic Disease Management Evidence-based Synthesis Program
138
Author, year Study design Type of Clinic
Target Population
Duration of
Study/ Follow-up
Inclusion/Exclusion Criteria
Goal of Intervention
Primary
Outcome
Type of Pharmacist Pharmacist Intervention Comparator
Intervention Collaboration
Okamoto 200175 RCT General medicine clinics within a managed care facility
HTN 6 months
Inclusion: -age ≥18 years -diagnosed with essential HTN -member of the managed care organization for ≥1 year -fill prescriptions at managed care organization’s pharmacies -taking targeted anti-HTN drugs nifedipine, verapamil, captopril, diltiazem, clonidine, terazosin, propranolol, or lisinopril, or taking ≥3 prescription anti-HTN drugs Exclusion: -secondary HTN (secondary to drugs or comorbid diseases including but not limited to CKD, cancer, Cushing’s syndrome, primary aldosteronism, or aortic coarctation) -significant end-organ disease (hospitalization likely within next few months) -baseline blood pressure > 200 mm Hg/105 mm Hg
BP control Difference in mean systolic and diastolic BPs, quality of life, costs
Clinical N=164 -Pharmacist
-informed patients that effort would be made to decrease number of drugs for HTN or alter therapy by administering more appropriate/less expensive drugs to achieve similar or improved BP control -determined most appropriate anti-HTN regimen for patient and ordered laboratory tests as needed -provided education on non-pharmacologic ways to control BP
Mode/Frequency: -visits at baseline and 6m -pharmacist and physician could schedule additional appointments if necessary
N=166 Usual care Physician- managed
Not reported
Solomon 199823 Gourley 199824 RCT Veterans Affairs Medical Center and university medical center
HTN 6 months
Inclusion: -age ≥18 years -receiving dihyropyridine or dihyropyridine and diuretic therapy for HTN Exclusion: -symptomatic heart failure -taking any anti-HTN agent other than dihyropyridine -evidence of alcohol or drug abuse -participated in investigational drug trial within 30 days of enrollment
Evaluate effects of pharmacy care on humanistic outcomes Compliance, knowledge, health resource use, QoL, satisfaction with care
Clinical N=63 Pharmacist care defined as -standardized patient assessment activities (physical assessment) -regularly scheduled therapeutic and educational interventions Mode/Frequency: -5 clinic visits, every 4 to 6 weeks
N=70 Usual care (traditional pharmacy care) (n=70)
Not reported
Pharmacist-led Chronic Disease Management Evidence-based Synthesis Program
139
Author, year Study design Type of Clinic
Target Population
Duration of
Study/ Follow-up
Inclusion/Exclusion Criteria
Goal of Intervention
Primary
Outcome
Type of Pharmacist Pharmacist Intervention Comparator
Intervention Collaboration
Erickson 199765 CCT University medical center
HTN 5 months
Inclusion: -age ≥18 years -read and speak English -diagnosis of essential HTN (baseline diastolic > 90 mm Hg and/or systolic > 140 mm Hg) documented on their medical record, and be -taking a prescribed antihypertensive drug Exclusion: -secondary HTN (drug induced, pheochromocytoma, chronic renal disease or renovascular disease, Cushing’s syndrome, primary aldosteronism, coarctation of the aorta)
BP control Primary outcome not specified
Clinical N=40 -Reviewed medical records -Took drug history including current and previous prescription and nonprescription therapy and presence of side effects -Assessed patient-specific drug issues (ie, access to pharmacy services, concerns and beliefs about taking drugs), prescription drug coverage; compliance; patient knowledge about hypertension, lifestyle modification, and drug therapy -Consulted with physicians about potential or observed drug-related problems -Counseled patients regarding new or continued drug therapy; reinforcing the importance of lifestyle modification -Monitored drug therapy via interview and laboratory data -Taking and/or interpreting blood pressure measurements Mode/Frequency: -Regularly scheduled clinic visits during study period
N=40 Usual care Not matched
Not reported
BP = blood pressure; CHF = congestive heart failure; CKD = chronic kidney disease; CV = cardiovascular; DM = diabetes mellitus; EMR= electronic medical record; ESRD = end-stage renal disease; HTN = hypertension; JNC V = Joint National Committee on Detection, Evaluation, and Treatment of High Blood Pressure; MI = myocardial infarction; NYHA = New York Heart Association; PACT = patient-aligned care team; PCMH = patient-centered medical home; PCP = primary care provider; QoL= quality of life
Pharmacist-led Chronic Disease Management Evidence-based Synthesis Program
140
Table 32. Drug-related Problems Outcomes – Hypertension Studies
Study Intervention (n) Control (n)
Inappropriate dosage/prescription or
omission % (n/N) Ineffectiveness% (n/N)
Drug-drug or drug-disease interaction (describe) %
(n/N)
Non-adherence to prescribed regimen
% (n/N) Clinical/adverse events %
(n/N)
Pharmacy Component Control Pharmacy
Component Control Pharmacy Component Control Pharmacy
Component Control Pharmacy Component Control
Carter 201561 IG=194 (Brief) IG=207 (Sustained) CG=224
NR NR NR NR NR NR NR NR No overall differences in the frequency of subjects reporting
any serious adverse event across the 3 groups
Zillich 201566 IG=465 CG=1,268
NR NR NR NR NR NR MPR at 12m All BP meds 0.71 (0.19)
MPR >/=80% at 12m all BP
meds 35%
0.71 (0.20) (P=.89)
32%
(P=.69)
NR NR
Hirsch 201469 IG=75 CG=91
Of patients with a drug problem:
Need for additional therapy Baseline
42% (14/33) 6 months
58% (7/12) 9 months 25% (1/4)
Need for dose increase Baseline
33% (11/33) 6 months
25% (3/12) 9 months 25% (1/4)
NR NR NR NR NR Of patients with a drug problem:
Non-adherence:
Baseline 15% (5/33) 6 months 8% (1/12) 9 months 25% (1/4)
NR Of patients with a drug problem:
Adverse drug reaction Baseline 6% (2/33) 6 months
16% (2/12) 9 months
0
NR
Magid 201370 IG=175 CG=173
NR NR NR NR NR NR Mean MPR Baseline 0.86
6m 0.87 (P=.93)
Adherence to home BP
monitoring 30% (49/162)
NR NR NR
Pharmacist-led Chronic Disease Management Evidence-based Synthesis Program
141
Study Intervention (n) Control (n)
Inappropriate dosage/prescription or
omission % (n/N) Ineffectiveness% (n/N)
Drug-drug or drug-disease interaction (describe) %
(n/N)
Non-adherence to prescribed regimen
% (n/N) Clinical/adverse events %
(n/N)
Pharmacy Component Control Pharmacy
Component Control Pharmacy Component Control Pharmacy
Component Control Pharmacy Component Control
Margolis 201362 IG=228 CG=222
NR NR NR NR NR NR 6 monthsa
23% 12 monthsa
31% 18 monthsa
28%
6 monthsa
39% (P=.04)
12 monthsa
36% (P=.33)
18 monthsa
37% (P=.06)
Total: 49 events
Hypotension, dizziness, or
loss of conscious: 6 events
HTN related: 1 event Stroke:
2 events Atrial
fibrillation: 1 event Angina: 1 event
Total: 60 events Allergic
reactions attributed to
HTN medicine: 2 events
Hypotension, dizziness, or
loss of conscious:
1 event HTN-related:
4 events Stroke:
5 events TIA:
3 events Atrial
fibrillation: 1 event
MI: 1 event Cardiac bypass surgery: 2 events
Magid 201167 IG=174 CG=164
NR NR NR NR NR NR 6 monthsa
30% 6 monthsa
31% (P=.93)
based on subset of
224 patients
NR NR
Carter 200963 IG=192 CG=210
NR NR NR NR NR NR Baseline 17%
(SD 28%) 6 months
15% (SD 25%)
Baseline 19%
(SD 22%) 6 months
15% (SD 21%) (P=.98)
NR NR
Pharmacist-led Chronic Disease Management Evidence-based Synthesis Program
142
Study Intervention (n) Control (n)
Inappropriate dosage/prescription or
omission % (n/N) Ineffectiveness% (n/N)
Drug-drug or drug-disease interaction (describe) %
(n/N)
Non-adherence to prescribed regimen
% (n/N) Clinical/adverse events %
(n/N)
Pharmacy Component Control Pharmacy
Component Control Pharmacy Component Control Pharmacy
Component Control Pharmacy Component Control
Carter 200864 IG=101 CG=78
NR NR NR NR NR NR Baseline 29%
9 monthsa
6%
Baseline 11%
9 monthsa
8% (P=.369)
Adverse event scoreb
Baseline 28.8
9 months 22.2
Adverse event scoreb
Baseline 26.5
9 months 18.3
(P=.135) Green 200871 IG=261 Home BP and Web only CG=259 Usual care CG=258 Ralston 201474 (sub-study) IG=186 CG=197 Home BP and Web
NR NR NR NR NR NR Adherence at least 80% 176/186 (95%)
179/197 (91%)
(P=.224) (Ralston
2014)
Nonfatal CV events
1% (3/261)
Nonfatal CV events
Usual care <1% (2/258) Home/web
only 1.5% (4/259) (Green 2008)
Hunt 200872 IG=230 CG=233
NR NR NR NR NR NR 12 monthsa
33% 12 monthsa
31% (P=.77)
NR NR
Vivian 200268 IG=27 CG=29
NR NR NR NR NR NR >90% of patients in both groups stated they took their
drugs as directed by their health care professional and
did not take more than prescribed (P=1.00)
-Forgot to take drug ≥1x/wk IG: 68% CG: 48% (P=.252)
NR NR
Okamoto 200175 IG=164 CG=166
NR NR NR NR NR NR NR NR None Reported
Cardiac problems 2 patients Headache 1 patient Dizziness 1 patient
Pharmacist-led Chronic Disease Management Evidence-based Synthesis Program
143
Study Intervention (n) Control (n)
Inappropriate dosage/prescription or
omission % (n/N) Ineffectiveness% (n/N)
Drug-drug or drug-disease interaction (describe) %
(n/N)
Non-adherence to prescribed regimen
% (n/N) Clinical/adverse events %
(n/N)
Pharmacy Component Control Pharmacy
Component Control Pharmacy Component Control Pharmacy
Component Control Pharmacy Component Control
Solomon 1998 Gourley 1998c
23,24 IG=63 CG=70
Drug needed not prescribed 1.6% (4/255 problems
identified by pharmacists)
Drug not needed but prescribed 0.4% (1/255) Dose problem 3.5% (9/255)
NR NR NR Risk of interaction
12.2% (31/255
problems identified by pharmacists)
NR Patient compliance
0.23d
Patient compliance
0.61d (P<.05)
NR by group NR by group
*All p-values versus control unless indicated. ARQ = Adverse reaction questionnaire; BP = blood pressure; CG = control group; CV = cardiovascular; IG = intervention group; MI = myocardial infarction; MPR = medication possession ratio; TIA = transient ischemic attacks a Values reported are the inverse of adherence to hypertension medication b Adverse reaction questionnaire included 47 questions of typical medication adverse effects; patient could rate the potential reaction as follows: 0 (not at all), 1 (a little bit), 2 (somewhat), 3 (quite a bit), or 4 (very much). The responses for each patient were summed (potential range, 0–188). c Drug problems or needs identified by pharmacist were reported but there were no comparator data d Mean sum score (1 point for every “yes” non-compliance item) based on a 4-item scale self-reported adherence measure
Pharmacist-led Chronic Disease Management Evidence-based Synthesis Program
144
Table 33. Mortality, Quality of Life, Access, and Patient Satisfaction Outcomes – Hypertension Studies
Study; Intervention (n) Control (n)
All-cause mortality % (n/N)
Health-related quality of life (describe) Access to care (describe) Patient satisfaction with care
(describe) Pharmacy
component Control Pharmacy component Control Pharmacy
component Control Pharmacy component Control
Hirsch 201469 IG=75 CG=91
NR NR NR NR NR NR Mean (SD) (0-100 scale with
higher # = higher satisfaction)
6 months 92.4 (10.9); n=49
9 months 92.7 (11.0); n=44
NR
Magid 201370 IG=175 CG=173
NR NR NR NR NR NR % very or completely
satisfied with HTN care
58% (102/175)
42% (73/173) P<.001a
Pharmacist-led Chronic Disease Management Evidence-based Synthesis Program
145
Study; Intervention (n) Control (n)
All-cause mortality % (n/N)
Health-related quality of life (describe) Access to care (describe) Patient satisfaction with care
(describe) Pharmacy
component Control Pharmacy component Control Pharmacy
component Control Pharmacy component Control
Margolis 201362 IG=228 CG=222
NR NR SF-12 Physical 0-100
mean (95% CI) Baseline
48.0 Change
6 monthsb -0.50 (-1.56, 0.56)
12 monthsb -0.84 (-2.0, 0.32)
18 monthsb -0.54 (-1.77, 0.69)
SF-12 Mental Baseline
52.2 6 monthsb
0.25 (-0.88, 1.38) 12 monthsb
-0.05 (-1.83, 0.78) 18 monthsb
1.51 (-0.18, 2.40)
SF-12 Physical 0-100, mean
(95% CI) Baseline
47.3 Change
6 monthsb -1.17 (-2.26, 0.07)
12 monthsb -0.72 (-1.90, 0.45)
18 monthsb -0.82 (-2.09, 0.45)
SF-12 Mental Baseline
51.2 6 monthsb
0.09 (-1.08, 1.26) 12 monthsb
-0.78 (-2.11, 0.55) 18 monthsb
0.50 (-0.83, 1.84)
Can communicate
with healthcare team:
mean (95% CI) Baseline:
4.4 (4.2-4.5) Change
6m: 0.08 (-0.02, 0.18)
12m: -0.02 (-0.13, 0.1)
18m: 0.11 (-0.01, 0.21)
Had problems getting needed
care: Mean (95% CI)
Baseline: 1.7 (1.5, 1.9)
Change 6m
0.15 (-0.09, 0.39) 12m
0.15 (-0.15,0 .45) 18m
0.07 (-0.22, 0.35)
Can communicate
with healthcare team:
Mean (95% CI) Baseline:
4.4 (4.2-4.5) Change
6m: -0.06 (-0.16-
0.04) 12m:
0.07 (-0.04-0.18) 18m:
0.09 (-0.01-0.2) Had problems getting needed
care: Mean (95% CI)
Baseline: 1.9 (1.6, 2.1)
Change 6m
0.18 (-0.07, 0.43) 12m
0.04 (-0.26, 0.35) 18m
0.05 (-0.24, 0.34)
CAHPS 0-5c Overall rating of
health care Baseline 4.3 (4.2,
4.4 Change
6 monthsb 0.27 (0.16, 0.39)
12 monthsb 0.22 (0.08, 0.35)
18 monthsb 0.26 (0.13, 0.38)
Baseline 4.3 (4.1, 4.4
Change 6 monthsb
0.11 (-0.01, 0.23) 12 monthsb
0.18 (0.14, 0.32) 18 monthsb
0.15 (0.03, 0.28)
Pharmacist-led Chronic Disease Management Evidence-based Synthesis Program
146
Study; Intervention (n) Control (n)
All-cause mortality % (n/N)
Health-related quality of life (describe) Access to care (describe) Patient satisfaction with care
(describe) Pharmacy
component Control Pharmacy component Control Pharmacy
component Control Pharmacy component Control
Green 200871 IG=261 Home BP and Web only CG=259 Usual care CG=258 Ralston 201474 IG=186 CG=197 (Home BP and Web)
<1% (1/261) Cardiac arrest
Usual care (0/258)
Home/web
only <1%
(2/259) cancer
SF-12 measures 0-100, 100
highest SF-12 General
health Baseline
67.1 (SD 20.4) 12 months 66.6 (22.2)
SF-12 Physical Baseline
80.6 (SD 27) 12 months 81.0 (26.5)
SF-12 Emotional Baseline
71.6 (SD 16.8) 12 months 71.7 (19.7)
SF-12 Gen. health Baseline
67.1 (SD 20.4) 12 months Usual care 66.7 (20.4)
Home/web only 66.6 (20.9)
SF-12 Physical Baseline
80.6 (SD 27) 12 months Usual care 78.1 (27.7)
Home/web only 77.7 (30.3)
SF-12 Emotional Baseline
71.6 (SD 16.8) 12 months Usual care 71.5 (17.7)
Home/web only 72.1 (16.8)
NR NR CAHPS 0-10c Baseline
7.9 (SD 1.5) 12 months 8.3 (1.4)
PACIC Overall Mean (SD)
3.3 (0.8)
Baseline 7.9 (SD 1.5) 12 months Usual care 8.1 (1.5)
Home/web only 8.1 (1.5)
(Green 2008)
2.5 (0.9) (P<.001)
(Ralston 2014)
Hunt 200872 IG=230 CG=233
NR NR MOS SF-36 Physical
41 Mental
45 General Health
44
Physical 42 (P=.12)
Mental 44 (P=.16)
General Health 42 (P=.01)
NR NR Overall satisfaction
8.6
8.5 (P=.75)
Vivian 200268 IG=27 CG=29
NR NR SF-36 No statistically significant differences
were noted between the 2 groups from baseline to end of study
NR NR Very satisfied with
pharmacy services
88% (23/26)
68% (18/27) (P=.098)
Pharmacist-led Chronic Disease Management Evidence-based Synthesis Program
147
Study; Intervention (n) Control (n)
All-cause mortality % (n/N)
Health-related quality of life (describe) Access to care (describe) Patient satisfaction with care
(describe) Pharmacy
component Control Pharmacy component Control Pharmacy
component Control Pharmacy component Control
Okamoto 200175 IG=164 CG=166
NR NR SF-36 Only statistically significant difference at
end of study was found in the role-physical domain. Scores were
significantly higher (P=0.03) in the Intervention group (78.5 vs. 70.7). No differences between groups for any
other scores
NR NR NR NR
Solomon 1998 Gourley 199823,24 IG=63 CG=70
NR NR No statistically significant differences were noted between the 2 groups on
QoL items
NR NR Greater satisfaction in the intervention group. Intervention group provided
more positive responses (significant differences in 8/10 items from the
Pharmaceutical Care Questionnaire) about their pharmacists compared with
controls Erickson 199765 IG=40 CG=40
NR NR Groups similar for SF-36 Health Survey scores
NR NR NR NR
CAHPS = Consumer Assessment of Healthcare Providers and Systems survey; CG = control group; IG = intervention group; PACIC = Patient Assessment of Chronic Illness Care; QoL = quality of life; SF-36 = Short-Form 36 a All p-values versus control unless indicated b Change from baseline (95% CI) c 0 worst, 5 best
Pharmacist-led Chronic Disease Management Evidence-based Synthesis Program
148
Table 34. Healthcare Utilization and Cost Outcomes – Hypertension Studies
Study; Intervention (n) Control (n)
Office visits (means (SD) unless otherwise
indicated)
Urgent care or / Emergency room (ER)
(means (SD) unless otherwise indicated)
Hospitalization (means (SD) unless otherwise indicated)
Medications (means (SD) unless otherwise
indicated) Costs or Other (describe)
Pharmacy component Control
Pharmacy component Control
Pharmacy component Control
Pharmacy component Control
Pharmacy component Control
Carter 201561 IG=194 (Brief) IG=207 (Sustained) CG=224
NR NR NR NR NR NR Dose increases or med additions First 9 months Brief: 3.1 (3.2)
Sustained: 2.7 (3.1)
At 12 months Sustained: 0.3 (0.8)
At 18 months Sustained: 0.4 (1.2)
At 24 months Sustained: 0.3 (0.9)
0.7 (1.0) (P<.001)
0.1 (0.5) (P=.25)
0.3 (0.7) (P=.31)
0.2 (0.5) (P=.21)
NR NR
Zillich 201566 IG=465 CG=1,268
NR NR NR NR NR NR Medication Changes during 12 month follow-
up: 4 types of BP
meds had more changes (P<.01) in case group; 3
types of med plus “others”
were non-significant
NR NR NR
Hirsch 201469 IG=75 CG=91
PCP visits Mean (SD)
1.8 (1.5)
PC and pharmacy 4.4 (1.9)
PCP visits Mean (SD)
4.2 (1.0) (P<.001)a
PC and pharmacy 4.2 (1.0) (P=.38)
NR NR NR NR NR NR NR NR
Pharmacist-led Chronic Disease Management Evidence-based Synthesis Program
149
Study; Intervention (n) Control (n)
Office visits (means (SD) unless otherwise
indicated)
Urgent care or / Emergency room (ER)
(means (SD) unless otherwise indicated)
Hospitalization (means (SD) unless otherwise indicated)
Medications (means (SD) unless otherwise
indicated) Costs or Other (describe)
Pharmacy component Control
Pharmacy component Control
Pharmacy component Control
Pharmacy component Control
Pharmacy component Control
Magid 201370 IG=175 CG=173
Mean (SD) 3.3 (2.5);
n=162
3.1 (2.3); n=164 (P=.16)
Mean(SD) 0.04 (0.19)
n=162
0.05 (0.23) n=164 (P=.44)
Mean (SD) 0.03 (0.17)
n=162
0.04 (0.20); n=164 (P=.57)
No medication 4% (6/162)
≥1 dose increase
43% (69/162)
≥1 medications added
70% (113/162)
No medication 9% (15/164)
(P=.05) ≥1 dose increase
12% (20/164) (P<.001)
≥1 medications added
25% (41/164) (P<.001)
NR NR
Margolis 201362 IG=228 CG=222
Pharmacist visits: 11.4 (SD 3.9)
NR NR NR non-CV hospital-izations noted as
most common adverse
event out of n=49 events
non-CV hospital-izations noted as
most common adverse
event out of n=60 events
Prescribed any HTN medication Baseline 77%
Change 6 monthsb
17% (13, 20) 12 monthsb
18% (13, 21) 18 monthsb
18% (14, 21); At months 6, 12,
18 95% were on
HTN medication
Baseline 73% Change
6 monthsb 6% (-2, 13)
(P<.01) 12 monthsb
7% (-0.8, 14) (P<.01)
18 monthsb 8% (-0.3, 14)
(P<.05) At months 6, 12,
18 79-81% were on HTN medication
Direct program
costs $1045 over
the 12-month period
NR
Magid 201167 IG=174 CG=164
NR NR NR NR NR NR # HTN med. classes
Baseline 2.1 Change
6 monthsb 0.3
Intensity of HTN med. regimenc Baseline 3.2 6 monthsb
0.6 (P=.008)
# HTN med. classes
Baseline 2.1 Change
6 monthsa 0.1 (P=.05)
Intensity of HTN med. regimenc Baseline 3.3 6 monthsb
0.2 (P=.008)
NR NR
Pharmacist-led Chronic Disease Management Evidence-based Synthesis Program
150
Study; Intervention (n) Control (n)
Office visits (means (SD) unless otherwise
indicated)
Urgent care or / Emergency room (ER)
(means (SD) unless otherwise indicated)
Hospitalization (means (SD) unless otherwise indicated)
Medications (means (SD) unless otherwise
indicated) Costs or Other (describe)
Pharmacy component Control
Pharmacy component Control
Pharmacy component Control
Pharmacy component Control
Pharmacy component Control
Carter 200963 IG=192 CG=210
NR NR NR NR NR NR Mean increase in # HTN meds. from baseline
1.1 # of HTN meds.
Baseline 1.3 6 months 2.4 (1.1)
Mean increase in # HTN meds. from baseline 0.3 (P<.001)
# of HTN meds. Baseline 1.9
6 months 2.2 (1.1) (P=.22)
NR NR
Carter 200864 IG=101 CG=78
NR NR NR NR NR NR # HTN meds. Baseline 1.5
9 months 2.4 (0.9)
# HTN meds. Baseline 1.4
9 months 1.9 (1.0) (P=.003)
NR NR
Green 200871 IG=261 Home BP and Web only CG=259 Usual care CG=258
PC visits 3.2
between groups Modest
significant decrease in
% of patients with office visits to specialist
in the intervention
group (P=.04) vs.
other groups
PC visits Usual care
3.2 Home/web
only 3.0
P=NS
NS between groups
NS between groups
# HTN med. classes
Baseline 1.64 12 months 2.16 (0.93) (P<.001)
compared to all controls
Aspirin use Baseline 49%
12 months 67% (149/222)
# HTN med. classes
Baseline 1.64 12 months Usual care 1.69 (0.85);
Home/web only 1.94 (0.91)
Aspirin use
Baseline 49% 12 months Usual care
53% (124/234) Home/web only 56% (131/234)
NR NR
Pharmacist-led Chronic Disease Management Evidence-based Synthesis Program
151
Study; Intervention (n) Control (n)
Office visits (means (SD) unless otherwise
indicated)
Urgent care or / Emergency room (ER)
(means (SD) unless otherwise indicated)
Hospitalization (means (SD) unless otherwise indicated)
Medications (means (SD) unless otherwise
indicated) Costs or Other (describe)
Pharmacy component Control
Pharmacy component Control
Pharmacy component Control
Pharmacy component Control
Pharmacy component Control
Hunt 200872 IG=230 CG=233
PCP 3.2 (2.7);
n=142 Total
7.2 (3.3) PC-HTN 1.8 (1.7)
Total-HTN 5.8 (2.6)
PCP 4.7 (3.1);
n=130 (P<.0001)
Total 4.9 (3.3)
(P<.0001) PC-HTN 2.9 (2.2)
(P<.0001) Total-HTN 3.1 (2.4)
(P<.0001)
NR NR NR NR # HTN meds. Mean (SD) 12 months
2.7 (1.2); n=142
# HTN meds. 12 months
2.4 (1.1); n=130 (P=.02)
Use of generic anti-HTN agent
51%
Use of generic
anti-HTN agent 40%
(P=.008)
Borenstein 200373 IG=98 CG=99
PC visits 3.4
Provider and pharmacy
8.0
PC visits 6.0 (P<.01)
Provider and pharmacy
6.6 (P=.06)
NR NR NR NR Patients receiving at least one first-line anti-
HTN agent Baseline
68% 12 months
80% (78/98) Change (P=.02)
Patients receiving at least one first-line anti-
HTN agent Baseline
60% 12 months
70% (69/99) Change (P=.02)
Average provider visit costs/patient
$160 Increase in drug costs
from baseline $11.31
Average provider
visit costs/pati
ent $195
(P=.04) Increase
in drug costs
from baseline
$4.25 (P=.12)
Vivian 200268 IG=27 CG=29
77% (20/27) had ≥1
appointment with
physician
63% (17/29) had
appointment with PCP
(P=0.372).
NR NR NR NR ACEI 69 (18/26)
NS for all other
HTN meds
ACEI 96 (26/27) (P=.052)
NS for all other HTN meds
NR NR
Pharmacist-led Chronic Disease Management Evidence-based Synthesis Program
152
Study; Intervention (n) Control (n)
Office visits (means (SD) unless otherwise
indicated)
Urgent care or / Emergency room (ER)
(means (SD) unless otherwise indicated)
Hospitalization (means (SD) unless otherwise indicated)
Medications (means (SD) unless otherwise
indicated) Costs or Other (describe)
Pharmacy component Control
Pharmacy component Control
Pharmacy component Control
Pharmacy component Control
Pharmacy component Control
Okamoto 200175 IG=164 CG=166
Clinic visits 5.25
Clinic visits 1.41
(P<.001)
None 4 patients No patient hospitalized during the study for
reasons related to BP
# HTN meds. Baseline
2.18 6 months
2.12
# HTN meds. Baseline
2.06 (P=.33) 6 months
2.2 (P=.67)
Drug costs/pt $112 ($153)
Clinic visit
costs $131 ($59)
Total cost/pt $243 ($169)
Drug costs/pt
$149 ($230) (P=.08)
Clinic visit costs
$74 ($89) (P<.001)
Total cost/pt $233
($267) (P=.71)
Erickson 199765 IG=40 CG=40
Clinic visits 4.1
Clinic visits 3.5 (P=.06)
NR NR NR NR Number of antihypertensive therapies prescribed per person similar
between groups
NR NR
ACEI = Angiotensin-converting enzyme inhibitor; CG = control group; CV cardiovascular; IG = intervention group; PC = primary care; PCP = primary care physician; pt = patient; SD = standard deviation a All p-values versus control unless indicated b Change from baseline (95% CI) c Intensity of hypertension medication regimen was based on patient report of medication regimen (specific medication and dosage) with confirmation by reviewing the pharmacy list available through the site’s electronic medical record or the pill bottles that patients brought to the visits. For each patient, an average intensity score was derived based on the sum of the medication intensity score divided by the number of antihypertensive medications prescribed.
Pharmacist-led Chronic Disease Management Evidence-based Synthesis Program
153
Table 35. Goal Attainment Outcomes – Hypertension Studies
Study; Intervention (n) Control (n)
Patient Goal Attainment definition Percentage of patients attaining goal % (n/N)
Pharmacy component Control Carter 201561 IG=194 (Brief) IG=207 (Sustained) CG=224
BP <140/90 mmHg or <130/80 mmHg for patients with DM or CKD
9 months: 43% in intervention groups 9 months: 34% OR 1.57 (0.99, 2.50) (P=.059)
Zillich 201566 IG=465 CG=1,268
BP <130/80 mmHg (DM or CKD) BP <140/90 mmHg (Other)
Baseline: 35% 6m: 57%
12m: 64%
Baseline: 49% (P<.0001) 6month: 57% OR 1.1 (0.9-1.3) (P=.28)
12month: 60% OR 1.3 (1.1-1.6) (P=<.01) Hirsch 201469 IG=75 CG=91
BP goal <140/<90 mm Hg; <130/<80 mm 41Hg with comorbid diabetes
Baseline 53% (40/75) 6 months 81% (60/74) 9 months 70% (50/71)
Baseline 46% (41/89) 6 months 44% (40/91) (P<.001) 9 months 52% (47/91) (P<.02)
Magid 201370 IG=175 CG=173
BP goal <140/<90 mm Hg; < 130/<80 mm Hg with comorbid diabetes or
CKD
Overall: 6 m 54% (95/175) DM/CKD: 6 m 52% (42/81)
6 months, Overall 35% (61/173) 6 months, DM/CKD 22% (19/88)
(P<.05) Margolis 201362 IG=228 CG=222
BP goal <140/<90 mm Hg; <130/<80 mm Hg with comorbid diabetes or
CKD
6 months 72% (148/206) 12 months 71% (141/198) 18 months 72% (135/188)
51% for patients attending all clinic visits at 6, 12,and 18 months
Differential change from baseline for patients attending all clinic visits (95% CI)
29.6 (13.1, 46.0)
6 months 45% (89/197) (P<.001) 12 months 53% (102/193) (P=.005) 18 months 57% (104/182) (P=.003)
21% for patients attending all clinic visits at 6, 12,and 18 months
Magid 201167 IG=174 CG=164
BP goal <140/<90 mm Hg; <130/<80 mmHg with comorbid diabetes or CKD
6 months 36% (49/136)
6 months 35% (51/145) (P=.89)
Carter 200963 IG=192 CG=210
BP control was <140/90 mm Hg; <130/ 80 mm Hg with comorbid diabetes or
CKD
6 months 64% (122/191) 6 months, non-diabetics 69%
6 months, diabetics 46%
6 months 30% (63/210) (P<.001) 6 months, non-diabetics 32% (P<.001)
6 months, diabetics 26% (P=.003) Carter 200864 IG=101 CG=78
BP control was <140/90 mm Hg; <130/ 80 mm Hg with comorbid diabetes or
CKD
9 months, Overall 89% (90/101);
9 months, non-diabetics 91% 9 months, diabetics 82%
9 months, Overall 53% (41/78);
9 months, non-diabetics 63% 9 months, diabetics 24%
(P<.001)
Pharmacist-led Chronic Disease Management Evidence-based Synthesis Program
154
Study; Intervention (n) Control (n)
Patient Goal Attainment definition Percentage of patients attaining goal % (n/N)
Pharmacy component Control Green 200871 IG=261 Home BP and Web only CG=259 Usual care CG=258
BP goal <140/<90 mm Hg 12 months 56% (133/237) (95% CI 49, 62%)
P<.01
Patients With Systolic BP at Baseline ≥160 mm Hg
54% (28/52) (95% CI 40, 67%) P<.01
12 months Usual care 31% (77/247) (95% CI 25,
37%) Home/web only 36% (89/246) (95% CI 30,
42%)
Patients With Systolic BP at Baseline ≥160 mm Hg
Usual care 20% (10/51) (95% CI 11, 33%) Home/web only 26% (12/47) (95% CI 15,
40%) Hunt 200872 IG=230 CG=233
Target BP was <140/90 mm Hg 12 months, last study visit 62% (88/142)
12 months, last study visit 44% (57/130)
(P=.003) Borenstein 200373 IG=98 CG=99
BP goal was <140/90 mm Hg for patients < 65 years of age; <160/90 mm Hg for
patients ≥65 years of age
12 months 60% (59/98) 12 months 43% (42/98) (P=.02)
Vivian 200268 IG=27 CG=29
BP below140/90 mm Hg 6 months 81% (21/26) 6 months 30% (8/27) (P=.001)
Erickson 199765 IG=40 CG=40
BP goal ≤140/≤90 mm Hg 5 months 45% (18/40) 5 months 30% (12/40) (P=.17)
CG = control group; IG = intervention group; DM = diabetes mellitus; CKD = chronic kidney disease; NR=not reported; OR = odds ratio
Pharmacist-led Chronic Disease Management Evidence-based Synthesis Program
155
Table 36. Study and Intervention Characteristics – Polypharmacy/High Risk Studies
Author, year Study design Type of Clinic
Target Population
Duration of study/ follow-up
Inclusion/ Exclusion Criteria
Goal of Intervention
Primary
Outcome
Type of pharmacist Pharmacist Intervention Comparator
intervention Collaboration
Lee 200677 FAME Cohort (phase 1) followed by RCT (phase 2) Outpatient general medicine service and Armed Forces Retirement Home (both Walter Reed Army Medical Center)
Older patients taking multiple medications 14 months 3 phases: -run-in phase: (n=200) 2 month run-in with no intervention; baseline adherence, BP, LDL determined -phase 1: (n=174) 6 month cohort, all patients received comprehensive program -Phase 2: (n=159) 6 month RCT (continuation of program or usual care)
Inclusion: -age 65 or older -taking at least 4 chronic medications per day Exclusion: -did not live independently (ie, nursing home or assisted living excluded) -serious medical conditions such that 1-year survival was unlikely
For RCT – determine maintenance of medication adherence after withdrawal of intervention Primary outcome: persistence of medication adherence
Clinical pharmacists
N=83 for RCT -Individualized medication education -Dispensing of medications in blister pack adherence aid -Follow-up every 2 months Mode/Frequency: -Run-in phase: initial visit -First phase: regular follow-up with clinical pharmacists every 2 months
N=76 for RCT Pre-study medication provision (no education, no blister packs)
Not reported
Pharmacist-led Chronic Disease Management Evidence-based Synthesis Program
156
Author, year Study design Type of Clinic
Target Population
Duration of study/ follow-up
Inclusion/ Exclusion Criteria
Goal of Intervention
Primary
Outcome
Type of pharmacist Pharmacist Intervention Comparator
intervention Collaboration
Taylor, 200378 RCT Community-based primary care (Family medicine) clinics affiliated with academic center (rural, high-poverty)
Adults at high risk for medication-related adverse events 12 months
Inclusion: -age ≥18 yrs -receive care at participating clinics -3 or more of these risk factors: a. 5 or more meds b. 12 or more doses/day c. 4 or more med changes past year d. 3 or more concurrent diseases e. history of medication non-compliance, f. drugs requiring therapeutic monitoring Exclusion: -cognitive impairment -history of missed office visits -scheduling conflicts -life expectancy < 1 year
Determine effect of pharmaceutical care on prevention, detection, and resolution of drug-related problems in high-risk patients in a rural community Primary outcome not specified
Clinical pharmacist
N=33 Usual medical care plus: -20-minute meeting with pharmacist before PCP visit -Evaluate therapy indication, effectiveness, dosage; correct/give practical directions; assess drug interactions, therapeutic duplication, duration of treatment, untreated indications, and expense -Review medical record for med-related problems -Chart review - ensure drugs and allergies documented -History to determine compliance; check for complications of therapies -Comprehensive individualized patient education (review of disease, importance of lifestyle modifications, drug info) -Monitor patients’ responses to drugs -Attempt to improve compliance through simplified dosing, teaching techniques like peak flow meter use, inhaler use, glucometer use, pill boxes Mode/Frequency: -20-minute meeting with pharmacist -Saw patients during follow-up visits
N=36 Usual medical care (no pharmacist intervention)
Therapeutic recommendations communicated to physicians orally or written notes
Pharmacist-led Chronic Disease Management Evidence-based Synthesis Program
157
Author, year Study design Type of Clinic
Target Population
Duration of study/ follow-up
Inclusion/ Exclusion Criteria
Goal of Intervention
Primary
Outcome
Type of pharmacist Pharmacist Intervention Comparator
intervention Collaboration
Malone et al, 2000 and 200179,80 RCT VA Medical Center primary care clinics
Adult ambulatory care patients at high risk for drug-related problems 12 months
Inclusion: -VAMC patient for ≥12 months, ongoing -3 or more of: a. 5 or more meds b. 12 or more doses/day c. 4 or more med changes past yr d. 3 or more concurrent diseases e. h/o med non-compliance f. drugs requiring therapeutic monitoring Exclusion: -participated in pharmacist-managed clinics past year -life expectancy <12 mo -psychiatry care -non-English speaker -visually impaired
“determine if clinical pharmacists could affect economic resource use and humanistic outcomes in a population of veterans identified to be at high risk to experience a medication-related problem” -economic Costs -HRQOL -patient satisfaction
Clinical pharmacist
N=523 -Pharmacists practiced within scope of practice of respective VAMC -Medical records reviewed and patients interviewed to optimize medication therapy -Assess appropriateness of medication therapy -Physical assessments, (eg, BP) -Establish goals of medication therapy -Assess medication compliance -Conduct in-office laboratory tests (eg, finger stick blood glucose) -Identify non-treated disease states that may benefit from pharmacological therapy -Check for drug interactions -Monitor meds for therapeutic effect and toxicity by requesting laboratory tests -Patient education -Refer patients to primary care physicians, specialists, and other health care providers -Depending on site and scope of practice, start, stop, or change medication therapy Mode/Frequency: -At least 3 visits with clinical pharmacist (most face-to-face, few telephone)
N=531 Primary care with physician; no pharmacist contact
“clinical pharmacists worked with physicians and other health care providers”
BP = blood pressure; ER = emergency room; h/o=history of; HRQOL = health related quality of life; LDL = low density lipoprotein cholesterol; MAI = medication appropriateness index; PCP = primary care provider; RCT = randomized controlled trial; VAMC = Veterans Affairs Medical Center
Pharmacist-led Chronic Disease Management Evidence-based Synthesis Program
158
Table 37. Drug-related Problems Outcomes – Polypharmacy/High Risk Studies
Study Intervention (n) Control (n)
Inappropriate dosage/prescription
or omission % (n/N)
Ineffectiveness% (n/N) Drug-drug or drug-disease interaction (describe) % (n/N)
Non-adherence to prescribed regimen
% (n/N) Clinical/adverse events
% (n/N)
Pharmacy component Control Pharmacy
component Control Pharmacy component Control
Pharmacy componen
t Control Pharmacy
component Control
Lee 200677 IG=83 CG=73
NR NR NR NR NR NR Mean (SD) adherence at end of
RCT 95.5% (7.7%)
69.1% (16.4%) (P<.001)
NR NR
Taylor 200378 IG=33 CG=36
Percent of prescriptions
that were inappropriate Inappropriate
dosage: Baseline:
63.3% (133/210
prescriptions) 12 months:
12.9% (20/155
prescriptions) Inappropriate
indication: Baseline:
33.3% (70/210
prescriptions)12 months
16.2% (25/155
prescriptions)
Inappropriate dosage:
Baseline: 62.3%
(129/207) 12 months:
63.8% (143/224) (P=NR)
Inappropriate indication: Baseline:
46.8% (97/207)
12 months: 48.2%
(108/224) (P=NR)
Baseline: 29.1% (61/210
prescriptions 12 months:
13.6% (21/155)
Baseline: 44.9%
(93/207 prescriptions) 12 months:
44.6% (100/224) (P=NR)
Drug-drug Baseline:
22.9% (48/210
prescriptions) 12 months:
5.8% (9/155)
Drug-disease Baseline:
18.6% (39/210)
12 months: 9.0%
(14/155)
Drug-drug Baseline:
17.9% (37/207 prescriptions) 12 months:
22.8% (51/224) (P=NR)
Drug-disease Baseline:
21.3% (44/207)
12 months: 19.6%
(44/224) (P=NR)
Mean compliance 12 months
100%
Mean compliance
(SD) 88.9 (6.3%)
(P=.115)
Patients with at least one “medication
misadventure” 12 months: 2.8% (4/33)
3.0% (3/36)
(P=.73)
CG = comparison group; IG = intervention group; NR = not reported; SD = standard deviation
Pharmacist-led Chronic Disease Management Evidence-based Synthesis Program
159
Table 38. Mortality, Quality of Life, Access, and Patient Satisfaction Outcomes – Polypharmacy/High Risk Studies
Study; Intervention (n) Control (n)
All-cause mortality % (n/N)
Health-related quality of life (describe) Access to care (describe) Patient satisfaction with care
(describe) Pharmacy
component Control Pharmacy component Control Pharmacy
component Control Pharmacy component Control
Taylor 200378 IG=33 CG=36
NR NR SF-36, groups similar (P values not reported)
NR NR Pharmacy related
satisfaction (reporting unclear)
81.9 (4.8)
89 (6.2) (P=.000)
Malone 2000, Malone 200179,80 IG=523 CG=531 randomized; 447 and 484 completed
NR NR SF-36, No clinically meaningful effect on HRQOL but evidence to
suggest a dose-response relationship.
NR NR There was no difference in patient satisfaction between groups at
baseline or over time.
CG = comparison group; HRQOL = health-related quality of life; IG = intervention group; NR = not reported; SD = standard deviation; SF-36 = Short-form 36
Pharmacist-led Chronic Disease Management Evidence-based Synthesis Program
160
Table 39. Healthcare Utilization and Cost Outcomes – Polypharmacy/High Risk Studies
Study; Intervention (n) Control (n)
Office visits Urgent care visits/
Emergency room (ER) visits
Hospitalizations Medications Costs or Other (describe)
Pharmacy componen
t Control
Pharmacy componen
t Control
Pharmacy componen
t Control
Pharmacy componen
t Control Pharmacy
component Control Lee 200677 IG=83 CG=73
NR NR NR NR NR NR Mean number of antihyper-tensives
used 2.6 (1.23)
2.61 (1.14) (P=.93)
NR NR
Taylor 200378 IG=33 CG=36
NR NR 4/33 (total)
Change from
previous 12 months: -12
6/36 (total)
Change from
previous 12 months: 0 (P=.044)
2/33 (total)
Change in hospitaliza-tions from
previous 12 months: -22
11/36 (total)
Change in hospitaliza-tions from
previous 12 months: 0 (P=.003)
Number of prescribed
medicationsmean (SD)
at 12 months: 4.7 (2.0)
Number of prescribed
medicationsmean (SD)
at 12 months: 6.2 (2.0) (P=.002)
Drug is not least
expensive of options
Baseline: 50%
(105/210 prescriptions) 12 months:
38.7% (60/155)
Baseline:
62.3% (129/207)
12 months: 60.3%
(135/224) (P=NR)
Malone 2000, Malone 200179,80 IG=523 CG=531 randomized; 447 and 484 completed
Before: mean (SD) 21.7 (21.0) After: 26.3
(20.8) Mean
increase 4.8
Before: mean 20.6
(17.2) After: 23.4
(20.5) Mean
increase 2.8
(P=.003)
NR NR Before: 0.34 (0.78)
After: 0.53 (0.98)
Mean increase
0.13
Before: 0.36 (0.81)
After: 0.57 (1.20)
Mean increase
0.19 (P=.29)
Before: Drug fills:
56.9 (40.0) Mean
increase 5.6
Before Drug fills:
53.2 (34.5) Mean
increase 4.0
(P=.12)
Mean cost (all costs:
clinic visits, drug, lab,
and hospitaliza-
tions) baseline: $4,927
After: $5,947 Mean
increase $1,020
Mean cost baseline $4,419 After
$5,732 Mean
increase $1,313 (P=.06)
CG = comparison group; IG = intervention group; NR = not reported; SD = standard deviation
Pharmacist-led Chronic Disease Management Evidence-based Synthesis Program
161
Table 40. Goal Attainment Outcomes – Polypharmacy/High Risk Studies
Study; Intervention (n) Control (n)
Patient Goal Attainment definition Percentage of patients attaining goal (n/N)
Pharmacy component Control Lee 200677 IG=83 CG=73
Medication adherence > 80% at end of RCT 97% (75/77) 22% (15/69) (P<.001)
Taylor 200378 IG=33 CG=36
Hypertension (goal ≤ 140/90 mmHg, or ≤135/80mmHg if diabetic)
Diabetes (HbA1c ≤7.5%)
Dyslipidemia (ATP III guidelines)
Anticoagulation (INR 2-3)
91.7% (22/24)
100% (13/13)
77.8% (14/19)
100% (4/4)
27.6% (8/29) (P<.005)
26.7% (5/16)
(P<.005)
5.9% (1/19) (P<.005)
16.7% (1/6)
(P=NS) ATP III = Adult Treatment Panel III; CG = comparison group; IG = intervention group; INR = International Normalized Ratio; NR = not reported; NS = not statistically significant; RCT = randomized controlled trial
Pharmacist-led Chronic Disease Management Evidence-based Synthesis Program
162
APPENDIX D. RISK OF BIAS TABLES Table 1. Risk of Bias for Cardiovascular Disease, Dyslipidemia, Chronic Obstructive Pulmonary Disease, and Chronic Kidney Disease Studies
Author, Year Randomized? Sequence Generation
Allocation Concealment
Risk of Bias from Confounding (non-randomized)
Blinding Incomplete Outcome Reporting
Selective Reporting
Overall
Cardiovascular Disease or Risk Factors for Cardiovascular Disease Taveira 201411 Y unclear unclear unclear low low Medium Irons 201212 N high high unclear low low High Coronary Artery Disease Spence 201413 N high high unclear low low High Olson 200914 Y low unclear unclear unclear low Medium Congestive Heart Failure Gattis 199915 Y low unclear low low low Low Murray 200716 Y low unclear low unclear low Medium Dyslipidemia Smith 201354 N high low unclear low low Medium Miller 200855 N high high unclear unclear low High Mazzolini 200556 N high high unclear low low High Straka 200557 N high high unclear low low High Ellis 200058 Y high low low high low Medium Bogden 199759 Y unclear unclear unclear low low Medium Konzem 199760 N low high unclear low high High Chronic Obstructive Pulmonary Disease Cooney 201520 Y low low low unclear low Low Aspinall 2012/201321,22
N unclear high unclear low low Medium
Solomon 199823 Gourley 199824
Y low unclear high unclear low Medium
Chronic Kidney Disease Pai 2009 (2 articles18)17
Y (pilot) low low unclear high high Medium
Bucaloiu 200719 N low high unclear low low Medium
Pharmacist-led Chronic Disease Management Evidence-based Synthesis Program
163
Table 2. Risk of Bias for Depression Studies
Author, Year Randomized? Sequence Generation
Allocation Concealment
Risk of Bias from Confounding (non-randomized)
Blinding Incomplete Outcome Reporting
Selective Reporting
Overall
Adler 200425 Y low low low high low Low Capoccia 200426 Y unclear unclear unclear low low Medium Finley 200328 Y unclear low low high low Medium Finley 200229 N high high low high low High
Table 3. Risk of Bias for Diabetes Studies
Author, Year Randomized? Sequence Generation
Allocation Concealment
Risk of Bias from confounding (non-randomized)
Blinding Incomplete Outcome Reporting
Selective Reporting
Overall
McAdam-Marx 201553
N low unclear unclear low low Medium
Rothman, 200539 Y low low low low low Low Skinner 201535 N low low unclear low low Low Chung, 201450 N high low unclear low low Medium Spence, 201413 N high low high low low Medium Brummel, 201346 N high high unclear low low High Ip, 201343 N unclear low unclear low low Medium Jacobs, 201238 Y low low unclear low low Low Salvo, 201249 N high unclear high low low Medium Cohen, 201132 Y unclear unclear unclear low low Medium Padiyara, 201145 N high low unclear low unclear Medium Pape, 201148 Y unclear unclear unclear high low Medium Taveira, 201130 Y low low unclear low low Low Heisler, 2010/201233,34 Y low low unclear low low Low
Jameson, 201036 Y low low unclear low low High Johnson, 201042 N high high unclear low low High Taveira, 201031 Y unclear unclear low low low Medium Fox, 200947 N high low unclear low low Medium Scott, 200640 Y low unclear unclear unclear low Medium Kelly, 200044 N high unclear unclear high low Medium Odegard, 200551 Y unclear unclear low high unclear Medium Shane-McWhorter, 200541
N unclear high unclear low low High
Pharmacist-led Chronic Disease Management Evidence-based Synthesis Program
164
Author, Year Randomized? Sequence Generation
Allocation Concealment
Risk of Bias from confounding (non-randomized)
Blinding Incomplete Outcome Reporting
Selective Reporting
Overall
Stroup, 200352 Y unclear unclear high low low Medium Jaber, 199637 Y unclear unclear high low low Medium
Table 4. Risk of Bias for Hypertension Studies
Author, Year Randomized? Sequence Generation
Allocation Concealment
Risk of Bias from confounding (non-randomized)
Blinding Incomplete Outcome Reporting
Selective Reporting
Overall
Carter 201561 Y unclear unclear unclear low low Medium Zillich 201566 N low low unclear low Low Low Hirsch, 201469 Y low unclear NA uncleara low low Medium Magid 201370 Y low unclear NA low low low Medium Margolis 201362 Y cluster unclear unclear NA high low low Medium Magid 201167 Y low unclear NA low low low Medium Carter 200963 Y cluster unclear unclear NA unclear low low Medium Carter 200864 Y cluster unclear unclear NA low low low Medium Green 200871 Y low low NA low low low Low Hunt 200872 Y low unclear NA low highb low Medium Borenstein 200373 Y unclear unclear NA unclear low low Medium
Vivian 200268 Y unclear unclear NA high low low Medium Okamoto 200175 Y unclear unclear NA unclear low low Medium Solomon 199823 Gourley 199824 Y low unclear NA high unclear low Medium
Erickson 199765 N high high unclear high low High a Potentially not blinded. Chart reviews were conducted by 2 clinical coordinators, one of whom was the study coordinator for this study. b Very high attrition
Pharmacist-led Chronic Disease Management Evidence-based Synthesis Program
165
Table 5. Risk of Bias for Polypharmacy Studies
Author, Year Randomized? Sequence Generation
Allocation Concealment
Risk of Bias from Confounding (non-randomized)
Blinding Incomplete Outcome Reporting
Selective Reporting
Overall
Polypharmacy/High Risk Lee 200677 Y (Phase 2) low low high low low Low Taylor 200378 Y unclear unclear unclear high low Medium Malone 2000 and 200179,80
Y low unclear low high low Medium